CA2767888A1 - Tamper-resistant dosage form for oxidation-sensitive opioids - Google Patents
Tamper-resistant dosage form for oxidation-sensitive opioids Download PDFInfo
- Publication number
- CA2767888A1 CA2767888A1 CA2767888A CA2767888A CA2767888A1 CA 2767888 A1 CA2767888 A1 CA 2767888A1 CA 2767888 A CA2767888 A CA 2767888A CA 2767888 A CA2767888 A CA 2767888A CA 2767888 A1 CA2767888 A1 CA 2767888A1
- Authority
- CA
- Canada
- Prior art keywords
- dosage form
- pharmaceutical dosage
- acid
- form according
- opioid
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Granted
Links
Classifications
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/33—Heterocyclic compounds
- A61K31/395—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins
- A61K31/435—Heterocyclic compounds having nitrogen as a ring hetero atom, e.g. guanethidine or rifamycins having six-membered rings with one nitrogen as the only ring hetero atom
- A61K31/47—Quinolines; Isoquinolines
- A61K31/485—Morphinan derivatives, e.g. morphine, codeine
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/20—Pills, tablets, discs, rods
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/20—Pills, tablets, discs, rods
- A61K9/2004—Excipients; Inactive ingredients
- A61K9/2013—Organic compounds, e.g. phospholipids, fats
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/20—Pills, tablets, discs, rods
- A61K9/2004—Excipients; Inactive ingredients
- A61K9/2022—Organic macromolecular compounds
- A61K9/2031—Organic macromolecular compounds obtained otherwise than by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyethylene glycol, polyethylene oxide, poloxamers
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/20—Pills, tablets, discs, rods
- A61K9/2004—Excipients; Inactive ingredients
- A61K9/2022—Organic macromolecular compounds
- A61K9/205—Polysaccharides, e.g. alginate, gums; Cyclodextrin
- A61K9/2054—Cellulose; Cellulose derivatives, e.g. hydroxypropyl methylcellulose
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/20—Pills, tablets, discs, rods
- A61K9/2095—Tabletting processes; Dosage units made by direct compression of powders or specially processed granules, by eliminating solvents, by melt-extrusion, by injection molding, by 3D printing
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/20—Pills, tablets, discs, rods
- A61K9/28—Dragees; Coated pills or tablets, e.g. with film or compression coating
- A61K9/2806—Coating materials
- A61K9/2833—Organic macromolecular compounds
- A61K9/284—Organic macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyvinyl pyrrolidone
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P25/00—Drugs for disorders of the nervous system
- A61P25/04—Centrally acting analgesics, e.g. opioids
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P25/00—Drugs for disorders of the nervous system
- A61P25/30—Drugs for disorders of the nervous system for treating abuse or dependence
Abstract
The invention relates to a thermoformed pharmaceutical dosage form having a breaking strength of at least 300 N, said dosage form comprising - an opioid (A), - - a free physiologically acceptable acid (B) in an amount of from 0T001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form, and - a polyalkylene oxide (C) having a weight average molecular weight Mw of at least 200,000 g/mol.
Description
Tamper-Resistant Dosage Form for Oxidation-Sensitive Opioids The invention relates to a pharmaceutical dosage form which contains an opioid with improved storage stability.
Many pharmacologically active compounds have a potential of being abused and thus, are advantageously provided in form of tamper resistant pharmaceutical dosage forms.
Prominent examples of such pharmacologically active compounds are opioids.
It is known that abusers crush conventional tablets, which contain opioids, to defeat the time-release "micro-encapsulation" and then ingest the resulting powder orally, intra-nasally, rectally, or by injection.
Various concepts for the avoidance of drug abuse have been developed. One concept relies on the mechanical properties of the pharmaceutical dosage forms, particularly an increased breaking strength (resistance to crushing). The major advantage of such pharmaceutical dosage forms is that comminuting, particularly pulverization, by conventional means, such as grinding in a mortar or fracturing by means of a hammer, is impossible or at least substantially impeded.
Such pharmaceutical dosage forms are useful for avoiding drug abuse of the pharmacolo-gically active compound contained therein, as they may not be powdered by conventional means and thus, cannot be administered in powdered from, e.g. nasally. The mechanical properties, particularly the high breaking strength of these pharmaceutical dosage forms renders them tamper resistant. In the context of such tamper resistant pharmaceutical dosage forms it can be referred to, e.g., WO 2005/016313, WO 2005/016314, WO
063214, WO 2005/102286, WO 2006/002883, WO 2006/002884, WO 2006/002886, WO
2006/082097, WO 2006/082099, and WO 2008/107149.
A problem in the manufacture of pharmaceutical dosage forms that contain opioids, such as oxymorphone, hydromorphone, and oxycodone, is their sensitivity towards oxidative degra-dation and decomposition. Oxidation may be caused by molecular oxygen or by radicals or peroxides generated by compounds that come into close proximity with these oxidation-CONFIRMATION COPY
Many pharmacologically active compounds have a potential of being abused and thus, are advantageously provided in form of tamper resistant pharmaceutical dosage forms.
Prominent examples of such pharmacologically active compounds are opioids.
It is known that abusers crush conventional tablets, which contain opioids, to defeat the time-release "micro-encapsulation" and then ingest the resulting powder orally, intra-nasally, rectally, or by injection.
Various concepts for the avoidance of drug abuse have been developed. One concept relies on the mechanical properties of the pharmaceutical dosage forms, particularly an increased breaking strength (resistance to crushing). The major advantage of such pharmaceutical dosage forms is that comminuting, particularly pulverization, by conventional means, such as grinding in a mortar or fracturing by means of a hammer, is impossible or at least substantially impeded.
Such pharmaceutical dosage forms are useful for avoiding drug abuse of the pharmacolo-gically active compound contained therein, as they may not be powdered by conventional means and thus, cannot be administered in powdered from, e.g. nasally. The mechanical properties, particularly the high breaking strength of these pharmaceutical dosage forms renders them tamper resistant. In the context of such tamper resistant pharmaceutical dosage forms it can be referred to, e.g., WO 2005/016313, WO 2005/016314, WO
063214, WO 2005/102286, WO 2006/002883, WO 2006/002884, WO 2006/002886, WO
2006/082097, WO 2006/082099, and WO 2008/107149.
A problem in the manufacture of pharmaceutical dosage forms that contain opioids, such as oxymorphone, hydromorphone, and oxycodone, is their sensitivity towards oxidative degra-dation and decomposition. Oxidation may be caused by molecular oxygen or by radicals or peroxides generated by compounds that come into close proximity with these oxidation-CONFIRMATION COPY
2 sensitive opioids. Pharmaceutical excipients as such, e.g. polyethylene glycols, may cause or catalyze oxidative degradation, for example in the course of the process for the manu-facture the pharmaceutical dosage forms. Further, molecular oxygen may generate said radicals or peroxides.
Typically, decomposition - is monitored-- in- standard -storage stability -tests e.g. - under accelerated storage conditions, such as 40 C / 75 % rel. humidity. Under these conditions, degradation and decomposition proceeds faster than under ambient conditions.
The drug approving authorities, such as CHMP and FDA, and international harmonization unions, such as ICH, have set standard storage stability thresholds which have to be met in order to get a pharmaceutical dosage form approved.
Particular problems arise when the oxidation-sensitive opioid needs to be exposed to ele-vated temperatures in the course of the manufacturing process, such as hot-melt extrusion, film coating and the like. Under these conditions the opioids are even more sensitive towards oxidation. For example, several known processes for the manufacture of pharmaceutical dosage forms having an increased breaking strength require that a pharmaceutical compo-sition containing the active ingredient is subjected to a specific amount of pressure at a specific elevated temperature for a specific period of time. Depending on the constituents of the pharmaceutical composition and their amounts, temperature, pressure and time may be varied within certain limits. However, if the minimal requirements are not satisfied, the breaking strength of the resultant pharmaceutical dosage form is too low.
In consequence, some conventional processes for the manufacture of pharmaceutical dosage forms, particularly for pharmaceutical dosage forms having an increased breaking strength, require comparatively harsh process conditions and thus, are so far not applicable for oxidation-sensitive opioids. In particular, chain rupture of pharmaceutical excipients such as polyethylene oxide during hot melt extrusion risks the formation of free radicals thereby further increasing the oxidative stress.
Lower dosages of oxidation-sensitive opioids often show a higher percentage of oxidative degradation and decomposition than higher dosages. Thus, as far as storage stability is concerned, pharmaceutical dosage forms containing lower dosages of oxidation-sensitive opioids need particular attention.
The effect of oxidation mechanisms and chemical interactions on stability of polymeric systems for amorphous A9-tetrahydrocannabinol (a non-opioid) produced by a hot-melt
Typically, decomposition - is monitored-- in- standard -storage stability -tests e.g. - under accelerated storage conditions, such as 40 C / 75 % rel. humidity. Under these conditions, degradation and decomposition proceeds faster than under ambient conditions.
The drug approving authorities, such as CHMP and FDA, and international harmonization unions, such as ICH, have set standard storage stability thresholds which have to be met in order to get a pharmaceutical dosage form approved.
Particular problems arise when the oxidation-sensitive opioid needs to be exposed to ele-vated temperatures in the course of the manufacturing process, such as hot-melt extrusion, film coating and the like. Under these conditions the opioids are even more sensitive towards oxidation. For example, several known processes for the manufacture of pharmaceutical dosage forms having an increased breaking strength require that a pharmaceutical compo-sition containing the active ingredient is subjected to a specific amount of pressure at a specific elevated temperature for a specific period of time. Depending on the constituents of the pharmaceutical composition and their amounts, temperature, pressure and time may be varied within certain limits. However, if the minimal requirements are not satisfied, the breaking strength of the resultant pharmaceutical dosage form is too low.
In consequence, some conventional processes for the manufacture of pharmaceutical dosage forms, particularly for pharmaceutical dosage forms having an increased breaking strength, require comparatively harsh process conditions and thus, are so far not applicable for oxidation-sensitive opioids. In particular, chain rupture of pharmaceutical excipients such as polyethylene oxide during hot melt extrusion risks the formation of free radicals thereby further increasing the oxidative stress.
Lower dosages of oxidation-sensitive opioids often show a higher percentage of oxidative degradation and decomposition than higher dosages. Thus, as far as storage stability is concerned, pharmaceutical dosage forms containing lower dosages of oxidation-sensitive opioids need particular attention.
The effect of oxidation mechanisms and chemical interactions on stability of polymeric systems for amorphous A9-tetrahydrocannabinol (a non-opioid) produced by a hot-melt
3 PCT/EP2010/004460 method is described in M. Munjal et al., J. Pharm. Sciences, 95(11), 2006, 2473-85. The study demonstrated for this highly unstable drug a complex nature of interactions including drug-excipient compatibility, use of antioxidants, cross-linking in polymeric matrixes, micro environment pH, and moisture effect.
K.C. Waterman-et al-., Pharm. Develop. Tech. 7(1-), 2002, 1-32 reviews the stabilization of pharmaceuticals to oxidative degradation. Various methods for reducing oxidation are recommended. The authors conclude that in the end, every drug presents a unique situation.
WO 2008/107149 discloses oral dosage forms having an increased breaking strength that may contain redox stabilizers such as complexing agents, e.g. EDTA.
K.C. Waterman-et al-., Pharm. Develop. Tech. 7(1-), 2002, 1-32 reviews the stabilization of pharmaceuticals to oxidative degradation. Various methods for reducing oxidation are recommended. The authors conclude that in the end, every drug presents a unique situation.
WO 2008/107149 discloses oral dosage forms having an increased breaking strength that may contain redox stabilizers such as complexing agents, e.g. EDTA.
4 relates to controlled release compositions containing a matrix composition comprising a) polymer or a mixture of polymers, b) an active drug substance and optionally c) one or more pharmaceutically acceptable excipients that is without alcohol induced dose dumping and have excellent properties with respect to avoiding drug abuse.
Preferably, the composition is resistant to isolate and/or dissolve the active drug substance from the composition by crushing, melting and/or ethanol extraction, whereby the composition is resistant to drug abuse. Citric acid may be present as flavouring agent.
Example 2 relates to a composition containing 7 wt.-% of citric acid.
WO 2008/148798 discloses an layered extended release composition for prolonged effect and a way to ensure prolonged effect e.g. once daily administration is to ensure optimal absorption of the active substance though the gastrointestinal tract i.e. from the stomach to rectum.
There is no general concept to successfully suppress oxidative degradation of oxidation-sensitive drugs in pharmaceutical dosage forms. The complex individual oxidation mechanisms that are relevant for a particular drug as well as the plurality of possible factors that have an influence on oxidation processes require extensive investigations in each particular case taking into account the particular circumstances.
It is further known that the other ingredients of the pharmaceutical dosage forms may show stability problems when being exposed to such harsh process conditions. For example, high molecular weight polyethylene oxide tends to degrade upon hot-melt extrusion.
Polymer degradation, however, may result in an uncontrolled release profile, particularly when the active ingredient is embedded in a matrix of the polyethylene oxide, and this might be another cause for oxidative degradation of the active ingredient by radicals.
When adding suitable excipients in order to stabilize the high molecular weight polyethylene oxide, such as a-tocopherol, it should be taken into considerations that said excipients in turn may have a detrimental effect on the stability of other ingredients of the pharmaceutical dosage, e.g. of the pharmacologically active compound.
It is an object of the present invention to provide tamper-resistant pharmaceutical dosage forms containing opioids, particularly oxidation-sensitive opioids, that have advantages over the pharmaceutical dosage forms of the prior art. The pharmaceutical dosage forms should have improved storage stability, so that they may contain oxidation-sensitive opioids even at comparatively low doses. Further, it should be possible to prepare the pharmaceutical dosage forms by conventional processes under conventional conditions such as elevated temperature and pressure (e.g. in the course of thermoforming by hot-melt extrusion).
This object has been solved by the subject-matter of the patent claims.
The invention relates to a thermoformed pharmaceutical dosage form having a breaking strength of at least 300 N and comprising - an opioid (A), - a free physiologically acceptable acid (B) in an amount of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form, and - a polyalkylene oxide (C) having a weight average molecular weight MW of at least 200,000 g/mol.
It has been surprisingly found that certain morphinan derivatives such as oxymorphone are oxidatively degraded to N-oxides (e.g., oxymorphone-N-oxide, N-oxides in general are often said to be toxic and possibly cancerogenic) upon manufacture and storage of the corres-ponding dosage forms and that the formation of said N-oxides and other decomposition products can be suppressed by the presence of suitable amounts of acid (B) in the pharmaceutical dosage forms according to the invention.
While it is not intended to be bound to any theory, the stabilizing effect of acid (B) might correlate with the pKA-value of the oxidation-sensitive opioids. The pKA-value of oxymor-phone is 8.3. Conventional formulations of oxymorphone, which are tamper resistant due to their increased breaking strength but which do not show the desired shelf life, give a pH
value of about 7.5 when being dispersed in water. Under these conditions, a considerable amount of the oxymorphone is present as a free base (i.e., is not protonated), which might be more sensitive towards oxidation than the (protonated) salt form. This concept is further supported by the fact that in the absence of acid (B), the dosage forms tend to have a yellowish, beige color, while the presence of acid (B) leads to whiter, e.g.
colorless tablets.
Thus, the presence of acid (B) might decrease the pH value within the dosage form thereby improving drug resistance towards oxidative degradation.
It has been surprisingly found that pharmaceutical excipients which are conventionally used in order to improve drug resistance towards oxidative degradation, particularly certain anti-oxidants, e.g., a-tocopherol, can be contra-productive and rather deteriorate than improve drug resistance towards oxidative degradation.
Furthermore, there is experimental evidence that surprisingly, acid (B) is also capable of stabilizing high molecular weight polyalkylene oxides against degradation, such as polyalkylene oxides (C) having a weight average molecular weight M, of at least 200,000 g/mol.
The pharmaceutical dosage form according to the invention is thermoformed, preferably by extrusion, although also other methods of thermoforming may be used in order to manufac-ture the pharmaceutical dosage form according to the invention such as press-molding at elevated temperature or heating of tablets that were manufactured by conventional compres-sion in a first step and then heated above the softening temperature of the polymer in the tablet in a second step to form hard tablets. In this regards, thermoforming means the forming, or molding of a mass after the application of heat. In a preferred embodiment, the pharmaceutical dosage form is thermoformed by hot-melt extrusion.
Preferably, the pharmaceutical dosage form is a monolithic mass. The pharmaceutical dosage form is preferably prepared by hot-melt extrusion. The melt extruded strands are preferably cut into monoliths, which are then preferably formed into tablets.
In this regard, the term "tablets" is preferably not to be understood as dosage forms being made by compres-sion of powder or granules (compressi) but rather, as shaped extrudates.
The pharmaceutical dosage form according to the invention contains, as component (A), an opioid (A), preferably an oxidation-sensitive opioid (A), most preferably oxymorphone or oxycodone. For the purpose of the specification, the term opioid (A) also includes the free base and the physiologically acceptable salts thereof.
According to the ATC index, opioids are divided into natural opium alkaloids, phenylpiperi-dine derivatives, diphenylpropylamine derivatives, benzomorphan derivatives, oripavine derivatives, morphinan derivatives and others. Examples of natural opium alkaloids are morphine, opium, hydromorphone, nicomorphine, oxycodone, dihydrocodeine, diamorphine, papaveretum, and codeine. Further opioids (A) are, for example, ethylmorphine, hydro-codone, oxymorphone, and the physiologically acceptable derivatives thereof or compounds, preferably the salts and solvates thereof, preferably the hydrochlorides thereof, physiolo-gically acceptable enantiomers, stereoisomers, diastereomers and racemates and the physiologically acceptable derivatives thereof, preferably ethers, esters or amides.
Further preferred opioids (A) include N-(1-methyl-2-piperidinoethyl)-N-(2-pyridyl)propion-amide, (1 R,2R)-3-(3-dimethylamino-1-ethyl-2-methyl-propyl)phenol, (1 R,2R,4S)-2-(dimethyl-amino)methyl-4-(p-fluorobenzyloxy)-1-(m-methoxyphenyl)cyclohexanol, (1R,2R)-3-(2-dime-thylaminomethyl-cyclohexyl)phenol, (1 S,2S)-3-(3-dimethylamino-1 -ethyl-2-methyl-propyl)-phenol, (2R,3R)-1-dimethylamino-3(3-methoxyphenyl)-2-methyl-pentan-3-ol, (1 RS,3RS,-6RS)-6-dimethylaminomethyl-1-(3-methoxyphenyl)-cyclohexane-1,3-diol, preferably as race-mate, 3-(2-d i methyla m inom ethyl- 1 -hyd roxy-cyclohexyl)phenyl 2-(4-isobutyl-phenyl)propio-nate, 3-(2-d i methyla m i nom ethyl- 1 -hyd roxy-cyclo hexyl)phe nyl 2-(6-methoxy-naphthalen-2-yl)-propionate, 3-(2-dimethylaminomethyl-cyclohex-1-enyl)-phenyl 2-(4-isobutyl-phenyl)propio-nate, 3-(2-dimethylaminomethyl-cyclohex-1 -enyl)-phenyl 2-(6-methoxy-naphthalen-2-yl)-propionate, (RR-SS)-2-acetoxy-4-trifluoromethyl-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hydroxy-4-trifluoromethyl-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-4-chloro-2-hydroxy-ben-zoic acid 3-(2-d i methyla m i nom ethyl- 1 -hyd roxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hydroxy-4-methyl-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hyd roxy-4-methoxy-benzoic acid 3-(2-d i methyla m i nom ethyl- 1 -hyd roxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hydroxy-5-nitro-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-2',4'-difluoro-3-hydroxy-biphenyl-4-carboxylic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, 1,1-(3-dimethylamino-3-phenyl-pentamethylen)-6-fluor-1,3,4,9-tetrahydropyrano[3,4-b]indole, in particular its hemicitrate;
1, 1 -[3-dimethylamino-3-(2-thienyl)pentamethylen]-1,3,4,9-tetrahydropyrano[3,4-b]indole, in particular its citrate; and 1,1-[3-dimethylamino-3-(2-thienyl)pentamethylen]-1,3,4,9-tetra-hydropyrano[3,4-b]-6-fluoro-indole, in particular its hemicitrate, and corresponding stereo-isomeric compounds, in each case the corresponding derivatives thereof, physiologically acceptable enantiomers, stereoisomers, diastereomers and racemates and the physiolo-gically acceptable derivatives thereof, e.g. ethers, esters or amides, and in each case the physiologically acceptable compounds thereof, in particular the salts thereof and solvates, e.g. hydrochlorides.
Preferred opioids (A) are of general formula (I) -N
R, wherein R, is -H, -OH or -OC,-6-alkyl;
R2 is -H or -C,-6-alkyl;
R3 is -H or -OH and R4 is -H; or R3 and R4 together are =0; and ---- is an optional double bond;
or the physiologically acceptable salts thereof.
Particularly preferred opioids (A) include oxymorphone, oxycodone, hydromorphone, and the physiologically acceptable salts thereof.
The content of the opioid (A) in the pharmaceutical dosage form is not limited.
Preferably, its content is within the range of from 0.01 to 80 wt.-%, more preferably 0.1 to 50 wt.-%, still more preferably 1 to 25 wt.-%, based on the total weight of the pharmaceutical dosage form. In a preferred embodiment, the content of opioid (A) is within the range of from 7 6 wt.-%, more preferably 7 5 wt.-%, still more preferably 5 4 wt.-%, 7 4 wt.-% or 9 4 wt.-%, most preferably 5 3 wt.-%, 7 3 wt.-% or 9 3 wt.-%, and in particular 5 2 wt.-%, 7 2 wt.-% or 9 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
In another preferred embodiment, the content of opioid (A) is within the range of from 11 10 wt.-%, more preferably 11 9 wt.-%, still more preferably 9 6 wt.-%, 11 6 wt.-%, 13 6 wt.-% or 15 6 wt.-%, most preferably 11 4 wt.-%, 13 4 wt.-% or 15 4 wt.-%, and in particular 11 2 wt.-%, 13 2 wt.-% or 15 2 wt.-%, based on the total weight of the pharmaceutical dosage form. In a further preferred embodiment, the content of opioid (A) is within the range of from 20 6 wt.-%, more preferably 20 5 wt.-%, still more preferably 20 4 wt.-%, most preferably 20 3 wt.-%, and in particular 20 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
Preferably, the total amount of the opioid (A) that is contained in the pharmaceutical dosage form is within the range of from 0.01 to 200 mg, more preferably 0.1 to 190 mg, still more preferably 1.0 to 180 mg, yet more preferably 1.5 to 160 mg, most preferably 2.0 to 100 mg and in particular 2.5 to 80 mg.
In a preferred embodiment, the opioid (A) is contained in the pharmaceutical dosage form in an amount of 7.5 5 mg, 10 5 mg, 20 5 mg, 30 5 mg, 40 5 mg, 50 5 mg, 60 5 mg, mg, 80 5 mg, 90 5 mg, 100 5 mg, 110 5 mg, 120 5 mg, 130 5, 140 5 mg, 150 5 mg, or 160 5 mg. In another preferred embodiment, the opioid (A) is contained in the pharma-ceutical dosage form in an amount of 5 2.5 mg, 7.5 2.5 mg, 10 2.5 mg, 15 2.5 mg, 20 2.5 mg, 25 2.5 mg, 30 2.5 mg, 35 2.5 mg, 40 2.5 mg, 45 2.5 mg, 50 2.5 mg, 55 2.5 mg, 60 2.5 mg, 65 2.5 mg, 70 2.5 mg, 75 2.5 mg, 80 2.5 mg, 85 2.5 mg, 90 2.5 mg, 95 2.5 mg, 100 2.5 mg, 105 2.5 mg, 110 2.5 mg, 115 2.5 mg, 120 2.5 mg, 125 2.5 mg, 130 2.5 mg, 135 2.5 mg, 140 2.5 mg, 145 2.5 mg, 150 2.5 mg, 155 2.5 mg, or 160 2.5 mg.
In a particularly preferred embodiment, opioid (A) is oxymorphone, preferably its HCI salt, and the pharmaceutical dosage form is adapted for administration twice daily.
In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 5 to 40 mg. In another particularly preferred embodiment, opioid (A) is oxymorphone, preferably its HCI, and the pharmaceutical dosage form is adapted for administration once daily. In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 10 to 80 mg.
In another particularly preferred embodiment, opioid (A) is oxycodone, preferably its HCI salt, and the pharmaceutical dosage form is adapted for administration twice daily.
In this embodi-ment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 5 to 80 mg. In another particularly preferred embodiment, opioid (A) is oxycodone, pre-ferably its HCI, and the pharmaceutical dosage form is adapted for administration once daily.
In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 10 to 320 mg.
In still another particularly preferred embodiment, opioid (A) is hydromorphone, preferably its HCI, and the pharmaceutical dosage form is adapted for administration twice daily. In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 2 to 52 mg. In another particularly preferred embodiment, opioid (A) is hydro-morphone, preferably its HCI, and the pharmaceutical dosage form is adapted for adminis-tration once daily. In this embodiment, opioid (A) is preferably contained in the pharmaceu-tical dosage form in an amount of from 4 to 104 mg.
The pharmaceutical dosage form according to the invention is characterized by excellent storage stability. Preferably, after storage for 4 weeks at 40 C and 75% rel.
humidity, the content of opioid (A) amounts to at least 98.0%, more preferably at least 98.5%, still more preferably at least 99.0%, yet more preferably at least 99.2%, most preferably at least 99.4%
and in particular at least 99.6%, of its original content before storage.
Suitable methods for measuring the content of the opioid (A) in the pharmaceutical dosage form are known to the skilled artisan. In this regard it is referred to the Eur. Ph. or the USP, especially to reversed phase HPLC analysis. Preferably, the pharmaceutical dosage form is stored in closed, preferably sealed containers, preferably as described in the experimental section, most preferably being equipped with an oxygen scavenger, in particular with an oxygen scavenger that is effective even at low relative humidity.
The pharmaceutical dosage form according to the invention contains, as component (B), a free physiologically acceptable acid in an amount of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form. The acid (B) may be organic or inorganic, liquid or solid. Solid acids are preferred, particularly crystalline organic or inorganic acids.
Acid (B) is free. This means that the acidic functional groups of the acid (B) are not all together constituents of a salt of the opioid (A). If the opioid (A) is present as a salt of an acid, e.g. as hydrochloride, the pharmaceutical dosage form according to the invention preferably contains as component (B) another, chemically different acid which is not present as a constituent of the salt of the opioid (A). In other words, monoacids that form a salt with opioid (A) are not to be considered as free acids (B) in the meaning of the present invention.
When acid (B) has more than a single acidic functional group (e.g. phosphoric acid), the acid (B) may be present as a constituent of a salt of the opioid (A), provided that at least one of the acidic functional groups of the acid (B) is not involved in the formation of the salt, i.e. is free. Preferably, however, each and every acidic functional group of acid (B) is not involved in the formation of a salt with opioid (A). It is also possible, however, that free acid (B) and the acid forming a salt with opioid (A) are identical. Under these circumstances the acid (B) is preferably present in molar excess compared to opioid (A).
In a preferred embodiment, the acid (B) contains at least one acidic functional group (e.g. -CO2H, -S03H, -P03H2, -OH and the like) having a pKA value within the range of 2.00 1.50, more preferably 2.00 1.25, still more preferably 2.00 1.00, yet more preferably 2.00 0.75, most preferably 2.00 0.50 and in particular 2.00 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 2.25 1.50, more preferably 2.25 1.25, still more preferably 2.25 1.00, yet more preferably 2.25 0.75, most preferably 2.25 0.50 and in particular 2.25 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 2.50 1.50, more preferably 2.50 1.25, still more preferably 2.50 1.00, yet more preferably 2.50 0.75, most preferably 2.50 0.50 and in particular 2.50 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA
value within the range of 2.75 1.50, more preferably 2.75 1.25, still more preferably 2.75 1.00, yet more preferably 2.75 0.75, most preferably 2.75 0.50 and in particular 2.75 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 3.00 1.50, more preferably 3.00 1.25, still more preferably 3.00 1.00, yet more preferably 3.00 0.75, most preferably 3.00 0.50 and in particular 3.00 0.25. In still another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 3.25 1.50, more preferably 3.25 1.25, still more preferably 3.25 1.00, yet more preferably 3.25 0.75, most preferably 3.25 0.50 and in particular 3.25 0.25.
In yet another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 4.50 1.50, more preferably 4.50 1.25, still more preferably 4.50 1.00, yet more preferably 4.50 0.75, most preferably 4.50 0.50 and in particular 4.50 0.25. In yet another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 4.75 1.50, more preferably 4.75 1.25, still more preferably 4.75 1.00, yet more preferably 4.75 0.75, most preferably 4.75 0.50 and in particular 4.75 0.25. In yet another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of
Preferably, the composition is resistant to isolate and/or dissolve the active drug substance from the composition by crushing, melting and/or ethanol extraction, whereby the composition is resistant to drug abuse. Citric acid may be present as flavouring agent.
Example 2 relates to a composition containing 7 wt.-% of citric acid.
WO 2008/148798 discloses an layered extended release composition for prolonged effect and a way to ensure prolonged effect e.g. once daily administration is to ensure optimal absorption of the active substance though the gastrointestinal tract i.e. from the stomach to rectum.
There is no general concept to successfully suppress oxidative degradation of oxidation-sensitive drugs in pharmaceutical dosage forms. The complex individual oxidation mechanisms that are relevant for a particular drug as well as the plurality of possible factors that have an influence on oxidation processes require extensive investigations in each particular case taking into account the particular circumstances.
It is further known that the other ingredients of the pharmaceutical dosage forms may show stability problems when being exposed to such harsh process conditions. For example, high molecular weight polyethylene oxide tends to degrade upon hot-melt extrusion.
Polymer degradation, however, may result in an uncontrolled release profile, particularly when the active ingredient is embedded in a matrix of the polyethylene oxide, and this might be another cause for oxidative degradation of the active ingredient by radicals.
When adding suitable excipients in order to stabilize the high molecular weight polyethylene oxide, such as a-tocopherol, it should be taken into considerations that said excipients in turn may have a detrimental effect on the stability of other ingredients of the pharmaceutical dosage, e.g. of the pharmacologically active compound.
It is an object of the present invention to provide tamper-resistant pharmaceutical dosage forms containing opioids, particularly oxidation-sensitive opioids, that have advantages over the pharmaceutical dosage forms of the prior art. The pharmaceutical dosage forms should have improved storage stability, so that they may contain oxidation-sensitive opioids even at comparatively low doses. Further, it should be possible to prepare the pharmaceutical dosage forms by conventional processes under conventional conditions such as elevated temperature and pressure (e.g. in the course of thermoforming by hot-melt extrusion).
This object has been solved by the subject-matter of the patent claims.
The invention relates to a thermoformed pharmaceutical dosage form having a breaking strength of at least 300 N and comprising - an opioid (A), - a free physiologically acceptable acid (B) in an amount of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form, and - a polyalkylene oxide (C) having a weight average molecular weight MW of at least 200,000 g/mol.
It has been surprisingly found that certain morphinan derivatives such as oxymorphone are oxidatively degraded to N-oxides (e.g., oxymorphone-N-oxide, N-oxides in general are often said to be toxic and possibly cancerogenic) upon manufacture and storage of the corres-ponding dosage forms and that the formation of said N-oxides and other decomposition products can be suppressed by the presence of suitable amounts of acid (B) in the pharmaceutical dosage forms according to the invention.
While it is not intended to be bound to any theory, the stabilizing effect of acid (B) might correlate with the pKA-value of the oxidation-sensitive opioids. The pKA-value of oxymor-phone is 8.3. Conventional formulations of oxymorphone, which are tamper resistant due to their increased breaking strength but which do not show the desired shelf life, give a pH
value of about 7.5 when being dispersed in water. Under these conditions, a considerable amount of the oxymorphone is present as a free base (i.e., is not protonated), which might be more sensitive towards oxidation than the (protonated) salt form. This concept is further supported by the fact that in the absence of acid (B), the dosage forms tend to have a yellowish, beige color, while the presence of acid (B) leads to whiter, e.g.
colorless tablets.
Thus, the presence of acid (B) might decrease the pH value within the dosage form thereby improving drug resistance towards oxidative degradation.
It has been surprisingly found that pharmaceutical excipients which are conventionally used in order to improve drug resistance towards oxidative degradation, particularly certain anti-oxidants, e.g., a-tocopherol, can be contra-productive and rather deteriorate than improve drug resistance towards oxidative degradation.
Furthermore, there is experimental evidence that surprisingly, acid (B) is also capable of stabilizing high molecular weight polyalkylene oxides against degradation, such as polyalkylene oxides (C) having a weight average molecular weight M, of at least 200,000 g/mol.
The pharmaceutical dosage form according to the invention is thermoformed, preferably by extrusion, although also other methods of thermoforming may be used in order to manufac-ture the pharmaceutical dosage form according to the invention such as press-molding at elevated temperature or heating of tablets that were manufactured by conventional compres-sion in a first step and then heated above the softening temperature of the polymer in the tablet in a second step to form hard tablets. In this regards, thermoforming means the forming, or molding of a mass after the application of heat. In a preferred embodiment, the pharmaceutical dosage form is thermoformed by hot-melt extrusion.
Preferably, the pharmaceutical dosage form is a monolithic mass. The pharmaceutical dosage form is preferably prepared by hot-melt extrusion. The melt extruded strands are preferably cut into monoliths, which are then preferably formed into tablets.
In this regard, the term "tablets" is preferably not to be understood as dosage forms being made by compres-sion of powder or granules (compressi) but rather, as shaped extrudates.
The pharmaceutical dosage form according to the invention contains, as component (A), an opioid (A), preferably an oxidation-sensitive opioid (A), most preferably oxymorphone or oxycodone. For the purpose of the specification, the term opioid (A) also includes the free base and the physiologically acceptable salts thereof.
According to the ATC index, opioids are divided into natural opium alkaloids, phenylpiperi-dine derivatives, diphenylpropylamine derivatives, benzomorphan derivatives, oripavine derivatives, morphinan derivatives and others. Examples of natural opium alkaloids are morphine, opium, hydromorphone, nicomorphine, oxycodone, dihydrocodeine, diamorphine, papaveretum, and codeine. Further opioids (A) are, for example, ethylmorphine, hydro-codone, oxymorphone, and the physiologically acceptable derivatives thereof or compounds, preferably the salts and solvates thereof, preferably the hydrochlorides thereof, physiolo-gically acceptable enantiomers, stereoisomers, diastereomers and racemates and the physiologically acceptable derivatives thereof, preferably ethers, esters or amides.
Further preferred opioids (A) include N-(1-methyl-2-piperidinoethyl)-N-(2-pyridyl)propion-amide, (1 R,2R)-3-(3-dimethylamino-1-ethyl-2-methyl-propyl)phenol, (1 R,2R,4S)-2-(dimethyl-amino)methyl-4-(p-fluorobenzyloxy)-1-(m-methoxyphenyl)cyclohexanol, (1R,2R)-3-(2-dime-thylaminomethyl-cyclohexyl)phenol, (1 S,2S)-3-(3-dimethylamino-1 -ethyl-2-methyl-propyl)-phenol, (2R,3R)-1-dimethylamino-3(3-methoxyphenyl)-2-methyl-pentan-3-ol, (1 RS,3RS,-6RS)-6-dimethylaminomethyl-1-(3-methoxyphenyl)-cyclohexane-1,3-diol, preferably as race-mate, 3-(2-d i methyla m inom ethyl- 1 -hyd roxy-cyclohexyl)phenyl 2-(4-isobutyl-phenyl)propio-nate, 3-(2-d i methyla m i nom ethyl- 1 -hyd roxy-cyclo hexyl)phe nyl 2-(6-methoxy-naphthalen-2-yl)-propionate, 3-(2-dimethylaminomethyl-cyclohex-1-enyl)-phenyl 2-(4-isobutyl-phenyl)propio-nate, 3-(2-dimethylaminomethyl-cyclohex-1 -enyl)-phenyl 2-(6-methoxy-naphthalen-2-yl)-propionate, (RR-SS)-2-acetoxy-4-trifluoromethyl-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hydroxy-4-trifluoromethyl-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-4-chloro-2-hydroxy-ben-zoic acid 3-(2-d i methyla m i nom ethyl- 1 -hyd roxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hydroxy-4-methyl-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hyd roxy-4-methoxy-benzoic acid 3-(2-d i methyla m i nom ethyl- 1 -hyd roxy-cyclohexyl)-phenyl ester, (RR-SS)-2-hydroxy-5-nitro-benzoic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, (RR-SS)-2',4'-difluoro-3-hydroxy-biphenyl-4-carboxylic acid 3-(2-dimethylaminomethyl-1-hydroxy-cyclohexyl)-phenyl ester, 1,1-(3-dimethylamino-3-phenyl-pentamethylen)-6-fluor-1,3,4,9-tetrahydropyrano[3,4-b]indole, in particular its hemicitrate;
1, 1 -[3-dimethylamino-3-(2-thienyl)pentamethylen]-1,3,4,9-tetrahydropyrano[3,4-b]indole, in particular its citrate; and 1,1-[3-dimethylamino-3-(2-thienyl)pentamethylen]-1,3,4,9-tetra-hydropyrano[3,4-b]-6-fluoro-indole, in particular its hemicitrate, and corresponding stereo-isomeric compounds, in each case the corresponding derivatives thereof, physiologically acceptable enantiomers, stereoisomers, diastereomers and racemates and the physiolo-gically acceptable derivatives thereof, e.g. ethers, esters or amides, and in each case the physiologically acceptable compounds thereof, in particular the salts thereof and solvates, e.g. hydrochlorides.
Preferred opioids (A) are of general formula (I) -N
R, wherein R, is -H, -OH or -OC,-6-alkyl;
R2 is -H or -C,-6-alkyl;
R3 is -H or -OH and R4 is -H; or R3 and R4 together are =0; and ---- is an optional double bond;
or the physiologically acceptable salts thereof.
Particularly preferred opioids (A) include oxymorphone, oxycodone, hydromorphone, and the physiologically acceptable salts thereof.
The content of the opioid (A) in the pharmaceutical dosage form is not limited.
Preferably, its content is within the range of from 0.01 to 80 wt.-%, more preferably 0.1 to 50 wt.-%, still more preferably 1 to 25 wt.-%, based on the total weight of the pharmaceutical dosage form. In a preferred embodiment, the content of opioid (A) is within the range of from 7 6 wt.-%, more preferably 7 5 wt.-%, still more preferably 5 4 wt.-%, 7 4 wt.-% or 9 4 wt.-%, most preferably 5 3 wt.-%, 7 3 wt.-% or 9 3 wt.-%, and in particular 5 2 wt.-%, 7 2 wt.-% or 9 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
In another preferred embodiment, the content of opioid (A) is within the range of from 11 10 wt.-%, more preferably 11 9 wt.-%, still more preferably 9 6 wt.-%, 11 6 wt.-%, 13 6 wt.-% or 15 6 wt.-%, most preferably 11 4 wt.-%, 13 4 wt.-% or 15 4 wt.-%, and in particular 11 2 wt.-%, 13 2 wt.-% or 15 2 wt.-%, based on the total weight of the pharmaceutical dosage form. In a further preferred embodiment, the content of opioid (A) is within the range of from 20 6 wt.-%, more preferably 20 5 wt.-%, still more preferably 20 4 wt.-%, most preferably 20 3 wt.-%, and in particular 20 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
Preferably, the total amount of the opioid (A) that is contained in the pharmaceutical dosage form is within the range of from 0.01 to 200 mg, more preferably 0.1 to 190 mg, still more preferably 1.0 to 180 mg, yet more preferably 1.5 to 160 mg, most preferably 2.0 to 100 mg and in particular 2.5 to 80 mg.
In a preferred embodiment, the opioid (A) is contained in the pharmaceutical dosage form in an amount of 7.5 5 mg, 10 5 mg, 20 5 mg, 30 5 mg, 40 5 mg, 50 5 mg, 60 5 mg, mg, 80 5 mg, 90 5 mg, 100 5 mg, 110 5 mg, 120 5 mg, 130 5, 140 5 mg, 150 5 mg, or 160 5 mg. In another preferred embodiment, the opioid (A) is contained in the pharma-ceutical dosage form in an amount of 5 2.5 mg, 7.5 2.5 mg, 10 2.5 mg, 15 2.5 mg, 20 2.5 mg, 25 2.5 mg, 30 2.5 mg, 35 2.5 mg, 40 2.5 mg, 45 2.5 mg, 50 2.5 mg, 55 2.5 mg, 60 2.5 mg, 65 2.5 mg, 70 2.5 mg, 75 2.5 mg, 80 2.5 mg, 85 2.5 mg, 90 2.5 mg, 95 2.5 mg, 100 2.5 mg, 105 2.5 mg, 110 2.5 mg, 115 2.5 mg, 120 2.5 mg, 125 2.5 mg, 130 2.5 mg, 135 2.5 mg, 140 2.5 mg, 145 2.5 mg, 150 2.5 mg, 155 2.5 mg, or 160 2.5 mg.
In a particularly preferred embodiment, opioid (A) is oxymorphone, preferably its HCI salt, and the pharmaceutical dosage form is adapted for administration twice daily.
In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 5 to 40 mg. In another particularly preferred embodiment, opioid (A) is oxymorphone, preferably its HCI, and the pharmaceutical dosage form is adapted for administration once daily. In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 10 to 80 mg.
In another particularly preferred embodiment, opioid (A) is oxycodone, preferably its HCI salt, and the pharmaceutical dosage form is adapted for administration twice daily.
In this embodi-ment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 5 to 80 mg. In another particularly preferred embodiment, opioid (A) is oxycodone, pre-ferably its HCI, and the pharmaceutical dosage form is adapted for administration once daily.
In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 10 to 320 mg.
In still another particularly preferred embodiment, opioid (A) is hydromorphone, preferably its HCI, and the pharmaceutical dosage form is adapted for administration twice daily. In this embodiment, opioid (A) is preferably contained in the pharmaceutical dosage form in an amount of from 2 to 52 mg. In another particularly preferred embodiment, opioid (A) is hydro-morphone, preferably its HCI, and the pharmaceutical dosage form is adapted for adminis-tration once daily. In this embodiment, opioid (A) is preferably contained in the pharmaceu-tical dosage form in an amount of from 4 to 104 mg.
The pharmaceutical dosage form according to the invention is characterized by excellent storage stability. Preferably, after storage for 4 weeks at 40 C and 75% rel.
humidity, the content of opioid (A) amounts to at least 98.0%, more preferably at least 98.5%, still more preferably at least 99.0%, yet more preferably at least 99.2%, most preferably at least 99.4%
and in particular at least 99.6%, of its original content before storage.
Suitable methods for measuring the content of the opioid (A) in the pharmaceutical dosage form are known to the skilled artisan. In this regard it is referred to the Eur. Ph. or the USP, especially to reversed phase HPLC analysis. Preferably, the pharmaceutical dosage form is stored in closed, preferably sealed containers, preferably as described in the experimental section, most preferably being equipped with an oxygen scavenger, in particular with an oxygen scavenger that is effective even at low relative humidity.
The pharmaceutical dosage form according to the invention contains, as component (B), a free physiologically acceptable acid in an amount of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form. The acid (B) may be organic or inorganic, liquid or solid. Solid acids are preferred, particularly crystalline organic or inorganic acids.
Acid (B) is free. This means that the acidic functional groups of the acid (B) are not all together constituents of a salt of the opioid (A). If the opioid (A) is present as a salt of an acid, e.g. as hydrochloride, the pharmaceutical dosage form according to the invention preferably contains as component (B) another, chemically different acid which is not present as a constituent of the salt of the opioid (A). In other words, monoacids that form a salt with opioid (A) are not to be considered as free acids (B) in the meaning of the present invention.
When acid (B) has more than a single acidic functional group (e.g. phosphoric acid), the acid (B) may be present as a constituent of a salt of the opioid (A), provided that at least one of the acidic functional groups of the acid (B) is not involved in the formation of the salt, i.e. is free. Preferably, however, each and every acidic functional group of acid (B) is not involved in the formation of a salt with opioid (A). It is also possible, however, that free acid (B) and the acid forming a salt with opioid (A) are identical. Under these circumstances the acid (B) is preferably present in molar excess compared to opioid (A).
In a preferred embodiment, the acid (B) contains at least one acidic functional group (e.g. -CO2H, -S03H, -P03H2, -OH and the like) having a pKA value within the range of 2.00 1.50, more preferably 2.00 1.25, still more preferably 2.00 1.00, yet more preferably 2.00 0.75, most preferably 2.00 0.50 and in particular 2.00 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 2.25 1.50, more preferably 2.25 1.25, still more preferably 2.25 1.00, yet more preferably 2.25 0.75, most preferably 2.25 0.50 and in particular 2.25 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 2.50 1.50, more preferably 2.50 1.25, still more preferably 2.50 1.00, yet more preferably 2.50 0.75, most preferably 2.50 0.50 and in particular 2.50 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA
value within the range of 2.75 1.50, more preferably 2.75 1.25, still more preferably 2.75 1.00, yet more preferably 2.75 0.75, most preferably 2.75 0.50 and in particular 2.75 0.25. In another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 3.00 1.50, more preferably 3.00 1.25, still more preferably 3.00 1.00, yet more preferably 3.00 0.75, most preferably 3.00 0.50 and in particular 3.00 0.25. In still another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 3.25 1.50, more preferably 3.25 1.25, still more preferably 3.25 1.00, yet more preferably 3.25 0.75, most preferably 3.25 0.50 and in particular 3.25 0.25.
In yet another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 4.50 1.50, more preferably 4.50 1.25, still more preferably 4.50 1.00, yet more preferably 4.50 0.75, most preferably 4.50 0.50 and in particular 4.50 0.25. In yet another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of 4.75 1.50, more preferably 4.75 1.25, still more preferably 4.75 1.00, yet more preferably 4.75 0.75, most preferably 4.75 0.50 and in particular 4.75 0.25. In yet another preferred embodiment, the acid (B) contains at least one acidic functional group having a pKA value within the range of
5.00 1.50, more preferably 5.00 1.25, still more preferably 5.00 1.00, yet more preferably 5.00 0.75, most preferably 5.00 0.50 and in particular 5.00 0.25.
Preferably, the acid (B) is an organic carboxylic or sulfonic acid, particularly a carboxylic acid.
Multicarboxylic acids and/or hydroxy-carboxylic acids are especially preferred.
In case of multicarboxylic acids, the partial salts thereof are also to be regarded as multi-carboxylic acids, e.g. the partial sodium, potassium or ammonium salts. For example, citric acid is a multicarboxylic acid having three carboxyl groups. As long as there remains at least one carboxyl group protonated (e.g. sodium dihydrogen citrate or disodium hydrogen citrate), the salt is to be regarded as a multicarboxylic acid. Preferably, however, all carboxyl groups of the multicarboxylic acid are protonated.
Preferably, the acid (B) is of low molecular weight, i.e., not polymerized.
Typically, the molecular weight of the acid (B) is below 500 g/mol.
Examples of acids include saturated and unsaturated monocarboxylic acids, saturated and -unsaturated- bicarboxylic acids, tricarboxylic acids, a-hydroxyacids and (3-hydroxylacids of monocarboxylic acids, a-hydroxyacids and (3-hydroxyacids of bicarboxylic acids, a-hydroxy-acids and (3-hydroxyacids of tricarboxylic acids, ketoacids, a-ketoacids, (3-ketoacids, of the polycarboxylic acids, of the polyhydroxy monocarboxylic acids, of the polyhydroxy bicar-boxylic acids, of the polyhydroxy tricarboxylic acids.
Preferably, the acid (B) is selected from the group consisting of benzenesulfonic acid, citric acid, a-glucoheptonic acid, D-gluconic acid, glycolic acid, lactic acid, malic acid, malonic acid, mandelic acid, propanoic acid, succinic acid, tartaric acid (d, I, or dl), tosic acid (toluenesulfonic acid), valeric acid, palmitic acid, pamoic acid, sebacic acid, stearic acid, lauric acid, acetic acid, adipic acid, glutaric acid, 4-chlorobenzenesulfonic acid, ethanedisulfonic acid, ethylsuccinic acid, fumaric acid, galactaric acid (mucic acid), D-glucuronic acid, 2-oxo-glutaric acid, glycerophosphoric acid, hippuric acid, isethionic acid (ethanolsulfonic acid), lactobionic acid, maleic acid, maleinic acid, 1,5-naphthalene-disulfonic acid, 2-naphthalene-sulfonic acid, pivalic acid, terephthalic acid, thiocyanic acid, cholic acid, n-dodecyl sulfate, 3-hydroxy-2-naphthoic acid, 1-hydroxy-2-naphthoic acid, oleic acid, undecylenic acid, ascorbic acid, (+)-camphoric acid, d-camphorsulfonic acid, dichloroacetic acid, ethanesulfonic acid, formic acid, methanesulfonic acid, nicotinic acid, orotic acid, oxalic acid, picric acid, L-pyroglutamic acid, saccharine, salicylic acid, gentisic acid, and/or 4-acetamidobenzoic acid.
The content of the acid (B) is within the range of from 0.001 to 5.0 wt.-%, preferably 0.005 to 2.5 wt.-%, more preferably 0.01 to 2.0 wt.-%, still more preferably 0.05 to 1.5 wt.-%, most preferably 0.1 to 1.0 wt.-% and in particular 0.2 to 0.9 wt.-%, based on the total weight of the pharmaceutical dosage form.
Preferably, the acid (B) is a multicarboxylic acid. More preferably, the multicarboxylic acid is selected from the group consisting of citric acid, maleic acid and fumaric acid.
Citric acid is particularly preferred.
The multicarboxylic acid, preferably citric acid, may be present in its anhydrous form or as a solvate and hydrate, respectively, e.g., as monohydrate.
In a preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.2 0.18 wt.-%, more preferably 0.2 0.15 wt.-%, still more preferably 0.2 0.12 wt.-%, yet more preferably 0.2 0.09 wt.-%, most preferably 0.2 0.06 wt.-%, and in particular 0.2 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.3 0.18 wt.-%, more preferably 0.3 0.15 wt.-%, still more preferably 0.3 0.12 wt.-%, yet more preferably 0.3 0.09 wt.-%, most preferably 0.3 0.06 wt.-%, and in particular 0.3 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In still another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.4 0.18 wt.-%, more preferably 0.4 0.15 wt.-%, still more preferably 0.4 0.12 wt.-%, yet more preferably 0.4 0.09 wt.-%, most preferably 0.4 0.06 wt.-%, and in particular 0.4 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.5 0.18 wt.-%, more preferably 0.5 0.15 wt.-%, still more preferably 0.5 0.12 wt.-%, yet more preferably 0.5 0.09 wt.-%, most preferably 0.5 0.06 wt.-%, and in particular 0.5 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.6 0.18 wt.-%, more preferably 0.6 0.15 wt.-%, still more preferably 0.6 0.12 wt.-%, yet more preferably 0.6 0.09 wt.-%, most preferably 0.6 0.06 wt.-%, and in particular 0.6 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.7 0.18 wt.-%, more preferably 0.7 0.15 wt.-%, still more preferably 0.7 0.12 wt.-%, yet more preferably 0.7 0.09 wt.-%, most preferably 0.7 0.06 wt.-%, and in particular 0.7 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of acid (B), preferably citric acid, is within the range of 0.8 0.18 wt.-%, more preferably 0.8 0.15 wt.-%, still more preferably 0.8 0.12 wt.-%, yet more preferably 0.8 0.09 wt.-%, most preferably 0.8 0.06 wt.-%, and in particular 0.8 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.85 0.18 wt.-%, more preferably 0.85 0.15 wt.-%, still more preferably 0.85 0.12 wt.-%, yet more preferably 0.85 0.09 wt.-%, most preferably 0.85 0.06 wt.-%, and in particular 0.85 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In still another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.9 0.18 wt.-%, more preferably 0.9 0.15 wt.-%, still more preferably 0.9 0.12 wt.-%, yet more preferably 0.9 0.09 wt.-%, most preferably 0.9 0.06 wt.-%, and in particular 0.9 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a further preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 1.0 0.18 wt.-%, more preferably 1.0 0.15 wt.-%, still more preferably 1.0 0.12 wt.-%, yet more preferably 1.0 0.09 wt.-%, most preferably 1.0 0.06 wt.-%, and in particular 1.0 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
The pharmaceutical dosage form according to the invention comprises, as component (C), a polyalkylene oxide (C) having a weight average molecular weight MW of at least 200,000 g/mol, preferably at least 500,000 g/mol, more preferably at least 750,000 g/mol, still more preferably at least 1,000,000 g/mol, most preferably at least 2,000,000 g/mol and in particular within the range of from 500,000 to 15,000,000 g/mol.
Preferably, the polyalkylene oxide is selected from the group consisting of polymethylene oxide, polyethylene oxide and polypropylene oxide, the copolymers and mixtures thereof.
Polyalkylene oxide (C) may comprise a single polyalkylene oxide having a particular average molecular weight, or a mixture (blend) of different polymers, such as two, three, four or five polymers, e.g., polymers of the same chemical nature but different average molecular weight, polymers of different chemical nature but same average molecular weight, or polymers of different chemical nature as well as different molecular weight.
For the purpose of the specification, a polyalkylene glycol has a molecular weight of up to 20,000 g/mol whereas a polyalkylene oxide has a molecular weight of more than 20,000 g/mol. In a preferred embodiment, the weight average over all molecular weights of all polyalkylene oxides that are contained in the pharmaceutical dosage form is at least 200,000 g/mol. Thus, polyalkylene glycols, if any, are preferably not taken into consideration when determining the weight average molecular weight of polyalkylene oxide (C).
Preferably, the content of the polyalkylene oxide (C) is within the range of from 20 to 99 wt.-%, more preferably 25 to 95 wt.-%, still more preferably 30 to 90 wt.-%, yet more preferably 30 to 85 wt.-%, most preferably 30 to 80 wt.-% and in particular 30 to 75 wt.-%, based on the total weight of the pharmaceutical dosage form. In a preferred embodiment, the content of the -polyalkylene oxide -is at least 20 wt.-%, more preferably at least 25 wt.-%, still more preferably at least 30 wt.-%, yet more preferably at least 35 wt.-% and in particular at least 40 wt.-%.
In a preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 25 20 wt.-%, more preferably 25 15 wt.-%, most preferably 25 10 wt.-%, and in particular 25 5 wt.-%. In another preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 35 20 wt.-%, more preferably 35 15 wt.-%, most preferably 35 10 wt.-%, and in particular 35 5 wt.-%. In still another preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 45 20 wt.-%, more preferably 45 15 wt.-%, most preferably 45 10 wt.-%, and in particular 45 5 wt.-%. In yet another preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 55 20 wt.-%, more prefer-ably 55 15 wt.-%, most preferably 55 10 wt.-%, and in particular 55 5 wt.-%.
In a further preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 65 20 wt.-%, more preferably 65 15 wt.-%, most preferably 65 10 wt.-%, and in particular 65 5 wt.-%. In still a further a preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 75 20 wt.-%, more preferably 75 15 wt.-%, most preferably 75 10 wt.-%, and in particular 75 5 wt.-%. In a still further a preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 80 15 wt.-%, more preferably 80 10 wt.-%, and most preferably 80 5 wt.-%.
In a preferred embodiment, polyalkylene oxide (C) is homogeneously distributed in the pharmaceutical dosage form according to the invention. Preferably, polyalkylene oxide (C) forms a matrix in which the opioid (A) is embedded. In a particularly preferred embodiment, the opioid (A) and polyalkylene oxide (C) are intimately homogeneously distributed in the pharmaceutical dosage form so that the pharmaceutical dosage form does not contain any segments where either opioid (A) is present in the absence of polyalkylene oxide (C) or where polyalkylene oxide (C) is present in the absence of opioid (A).
When the pharmaceutical dosage form is film coated, the polyalkylene oxide (C) is preferably homogeneously distributed in the core of the pharmaceutical dosage form, i.e.
the film coating preferably does not contain polyalkylene oxide (C). Nonetheless, the film coating as such may of course contain one or more polymers, which however, preferably differ from the polyalkylene oxide (C) contained in the core.
The polyalkylene oxide (C) may be combined with one or more different polymers selected from the group consisting of polyalkylene oxide, preferably polymethylene oxide, polyethy-lene oxide, polypropylene oxide; polyethylene, polypropylene, polyvinyl chloride, polycarbo-nate, polystyrene, polyvinylpyrrolidone, poly(alk)acrylate, poly(hydroxy fatty acids), such as for example poly(3-hydroxybutyrate-co-3-hydroxyvalerate) (Biopol ), poly(hydroxyvaleric acid); polycaprolactone, polyvinyl alcohol, polyesteramide, polyethylene succinate, polylac-tone, polyglycolide, polyurethane, polyamide, polylactide, polyacetal (for example poly-saccharides optionally with modified side chains), polylactide/glycolide, polylactone, poly-glycolide, polyorthoester, polyanhydride, block polymers of polyethylene glycol and polybuty-lene terephthalate (Polyactive ), polyanhydride (Polifeprosan), copolymers thereof, block-copolymers thereof, and mixtures of at least two of the stated polymers, or other polymers with the above characteristics.
Preferably, the molecular weight dispersity M,N/Mõ of polyalkylene oxide (C) is within the range of 2.5 2.0, more preferably 2.5 1.5, still more preferably 2.5 1.0, yet more preferably 2.5 0.8, most preferably 2.5 0.6, and in particular 2.5 0.4.
The polyalkylene oxide (C) preferably has a viscosity at 25 C of 30 to 17,600 cP, more preferably 55 to 17,600 cP, still more preferably 600 to 17,600 cP and most preferably 4,500 to 17,600 cP, measured in a 5 wt.-% aqueous solution using a model RVF
Brookfield viscosimeter (spindle no. 2 / rotational speed 2 rpm); of 400 to 4,000 cP, more preferably 400 to 800 cP or 2,000 to 4,000 cP, measured on a 2 wt.-% aqueous solution using the stated viscosimeter (spindle no. 1 or 3 / rotational speed 10 rpm); or of 1,650 to 10,000 cP, more preferably 1,650 to 5,500 cP, 5,500 to 7,500 cP or 7,500 to 10,000 cP, measured on a 1 wt.-% aqueous solution using the stated viscosimeter (spindle no. 2 / rotational speed 2 rpm).
In a preferred embodiment according to the invention the polyalkylene oxide (C) having a weight average molecular weight of at least 200,000 g/mol is combined with at least one further polymer, preferably but not necessarily also having a weight average molecular weight (Mw) of at least 200,000 g/mol, selected from the group consisting of polyethylene, polypropylene, polyvinyl chloride, polycarbonate, polystyrene, polyacrylate, poly(hydroxy fatty acids), polycaprolactone, polyvinyl alcohol, polyesteramide, polyethylene succinate, poly-lactone, polyglycolide, polyurethane, polyvinylpyrrolidone, polyamide, polylactide, polylactide/
glycolide, polylactone, polyglycolide, polyorthoester, polyanhydride, block polymers of polyethylene glycol and polybutylene terephthalate, polyanhydride, polyacetal, cellulose esters, cellulose ethers and copolymers thereof. Cellulose esters and cellulose ethers are particularly preferred, e.g. methylcelIulose, ethylcellulose, hydroxymethylcelIulose, hydroxy-ethylcellulose, hydroxypropylcellulose hydroxypropylmethylcellulose, ca rboxymethylcel I u lose, and the like.
In a preferred embodiment, said further polymer is neither a polyalkylene oxide nor a poly-alkylene glycol. Nonetheless, the pharmaceutical dosage form may contain polyalkylene glycol, e.g. as plasticizer, but then, the pharmaceutical dosage form preferably is a ternary mixture of polymers: polyalkylene oxide (C) + further polymer + plasticizer.
In a particularly preferred embodiment, said further polymer is a hydrophilic cellulose ester or cellulose ether, preferably hydroxypropylmethylcellulose (HPMC), hydroxypropylcellulose (HPC) or hyd roxyeth ylcel I u lose (HEC), preferably having an average viscosity (preferably measured by capillary viscosimetry or rotational viscosimetry) of 1,000 to 150,000 mPas, more preferably 3,000 to 150,000. In a preferred embodiment, the average viscosity is within the range of 110,000 50,000 mPas, more preferably 110,000 40,000 mPas, still more preferably 110,000 30,000 mPas, most preferably 110,000 20,000 mPas, and in particular 100,000 10,000 mPas.
In a preferred embodiment the relative weight ratio of said polyalkylene oxide (C) and said further polymer is within the range of from 20:1 to 1:20, more preferably 10:1 to 1:10, still more preferably 7:1 to 1:5, yet more preferably 5:1 to 1:1, most preferably 4:1 to 1,5:1 and in particular 3:1 to 2:1. In a preferred embodiment, the relative weight ratio of said polyalkylene oxide (C) and said further polymer is within the range of from 10:1 to 5:1, more preferably 8:1 to 5:1, most preferably 7:1 to 5:1.
Preferably, the content of said further polymer amounts to 0.5 to 25 wt.-%, more preferably 1.0 to 20 wt.-%, still more preferably 2.0 to 22.5 wt.-%, yet more preferably 3.0 to 20 wt.-%
and most preferably 4.0 to 17.5 wt.-% and in particular 5.0 to 15 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the further polymer is a cellulose ester or cellulose ether, prefer-ably HPMC, having a content within the range of 10 8 wt.-%, more preferably 10
Preferably, the acid (B) is an organic carboxylic or sulfonic acid, particularly a carboxylic acid.
Multicarboxylic acids and/or hydroxy-carboxylic acids are especially preferred.
In case of multicarboxylic acids, the partial salts thereof are also to be regarded as multi-carboxylic acids, e.g. the partial sodium, potassium or ammonium salts. For example, citric acid is a multicarboxylic acid having three carboxyl groups. As long as there remains at least one carboxyl group protonated (e.g. sodium dihydrogen citrate or disodium hydrogen citrate), the salt is to be regarded as a multicarboxylic acid. Preferably, however, all carboxyl groups of the multicarboxylic acid are protonated.
Preferably, the acid (B) is of low molecular weight, i.e., not polymerized.
Typically, the molecular weight of the acid (B) is below 500 g/mol.
Examples of acids include saturated and unsaturated monocarboxylic acids, saturated and -unsaturated- bicarboxylic acids, tricarboxylic acids, a-hydroxyacids and (3-hydroxylacids of monocarboxylic acids, a-hydroxyacids and (3-hydroxyacids of bicarboxylic acids, a-hydroxy-acids and (3-hydroxyacids of tricarboxylic acids, ketoacids, a-ketoacids, (3-ketoacids, of the polycarboxylic acids, of the polyhydroxy monocarboxylic acids, of the polyhydroxy bicar-boxylic acids, of the polyhydroxy tricarboxylic acids.
Preferably, the acid (B) is selected from the group consisting of benzenesulfonic acid, citric acid, a-glucoheptonic acid, D-gluconic acid, glycolic acid, lactic acid, malic acid, malonic acid, mandelic acid, propanoic acid, succinic acid, tartaric acid (d, I, or dl), tosic acid (toluenesulfonic acid), valeric acid, palmitic acid, pamoic acid, sebacic acid, stearic acid, lauric acid, acetic acid, adipic acid, glutaric acid, 4-chlorobenzenesulfonic acid, ethanedisulfonic acid, ethylsuccinic acid, fumaric acid, galactaric acid (mucic acid), D-glucuronic acid, 2-oxo-glutaric acid, glycerophosphoric acid, hippuric acid, isethionic acid (ethanolsulfonic acid), lactobionic acid, maleic acid, maleinic acid, 1,5-naphthalene-disulfonic acid, 2-naphthalene-sulfonic acid, pivalic acid, terephthalic acid, thiocyanic acid, cholic acid, n-dodecyl sulfate, 3-hydroxy-2-naphthoic acid, 1-hydroxy-2-naphthoic acid, oleic acid, undecylenic acid, ascorbic acid, (+)-camphoric acid, d-camphorsulfonic acid, dichloroacetic acid, ethanesulfonic acid, formic acid, methanesulfonic acid, nicotinic acid, orotic acid, oxalic acid, picric acid, L-pyroglutamic acid, saccharine, salicylic acid, gentisic acid, and/or 4-acetamidobenzoic acid.
The content of the acid (B) is within the range of from 0.001 to 5.0 wt.-%, preferably 0.005 to 2.5 wt.-%, more preferably 0.01 to 2.0 wt.-%, still more preferably 0.05 to 1.5 wt.-%, most preferably 0.1 to 1.0 wt.-% and in particular 0.2 to 0.9 wt.-%, based on the total weight of the pharmaceutical dosage form.
Preferably, the acid (B) is a multicarboxylic acid. More preferably, the multicarboxylic acid is selected from the group consisting of citric acid, maleic acid and fumaric acid.
Citric acid is particularly preferred.
The multicarboxylic acid, preferably citric acid, may be present in its anhydrous form or as a solvate and hydrate, respectively, e.g., as monohydrate.
In a preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.2 0.18 wt.-%, more preferably 0.2 0.15 wt.-%, still more preferably 0.2 0.12 wt.-%, yet more preferably 0.2 0.09 wt.-%, most preferably 0.2 0.06 wt.-%, and in particular 0.2 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.3 0.18 wt.-%, more preferably 0.3 0.15 wt.-%, still more preferably 0.3 0.12 wt.-%, yet more preferably 0.3 0.09 wt.-%, most preferably 0.3 0.06 wt.-%, and in particular 0.3 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In still another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.4 0.18 wt.-%, more preferably 0.4 0.15 wt.-%, still more preferably 0.4 0.12 wt.-%, yet more preferably 0.4 0.09 wt.-%, most preferably 0.4 0.06 wt.-%, and in particular 0.4 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.5 0.18 wt.-%, more preferably 0.5 0.15 wt.-%, still more preferably 0.5 0.12 wt.-%, yet more preferably 0.5 0.09 wt.-%, most preferably 0.5 0.06 wt.-%, and in particular 0.5 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.6 0.18 wt.-%, more preferably 0.6 0.15 wt.-%, still more preferably 0.6 0.12 wt.-%, yet more preferably 0.6 0.09 wt.-%, most preferably 0.6 0.06 wt.-%, and in particular 0.6 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.7 0.18 wt.-%, more preferably 0.7 0.15 wt.-%, still more preferably 0.7 0.12 wt.-%, yet more preferably 0.7 0.09 wt.-%, most preferably 0.7 0.06 wt.-%, and in particular 0.7 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of acid (B), preferably citric acid, is within the range of 0.8 0.18 wt.-%, more preferably 0.8 0.15 wt.-%, still more preferably 0.8 0.12 wt.-%, yet more preferably 0.8 0.09 wt.-%, most preferably 0.8 0.06 wt.-%, and in particular 0.8 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In yet another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.85 0.18 wt.-%, more preferably 0.85 0.15 wt.-%, still more preferably 0.85 0.12 wt.-%, yet more preferably 0.85 0.09 wt.-%, most preferably 0.85 0.06 wt.-%, and in particular 0.85 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In still another preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 0.9 0.18 wt.-%, more preferably 0.9 0.15 wt.-%, still more preferably 0.9 0.12 wt.-%, yet more preferably 0.9 0.09 wt.-%, most preferably 0.9 0.06 wt.-%, and in particular 0.9 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a further preferred embodiment, the content of the acid (B), preferably citric acid, is within the range of 1.0 0.18 wt.-%, more preferably 1.0 0.15 wt.-%, still more preferably 1.0 0.12 wt.-%, yet more preferably 1.0 0.09 wt.-%, most preferably 1.0 0.06 wt.-%, and in particular 1.0 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
The pharmaceutical dosage form according to the invention comprises, as component (C), a polyalkylene oxide (C) having a weight average molecular weight MW of at least 200,000 g/mol, preferably at least 500,000 g/mol, more preferably at least 750,000 g/mol, still more preferably at least 1,000,000 g/mol, most preferably at least 2,000,000 g/mol and in particular within the range of from 500,000 to 15,000,000 g/mol.
Preferably, the polyalkylene oxide is selected from the group consisting of polymethylene oxide, polyethylene oxide and polypropylene oxide, the copolymers and mixtures thereof.
Polyalkylene oxide (C) may comprise a single polyalkylene oxide having a particular average molecular weight, or a mixture (blend) of different polymers, such as two, three, four or five polymers, e.g., polymers of the same chemical nature but different average molecular weight, polymers of different chemical nature but same average molecular weight, or polymers of different chemical nature as well as different molecular weight.
For the purpose of the specification, a polyalkylene glycol has a molecular weight of up to 20,000 g/mol whereas a polyalkylene oxide has a molecular weight of more than 20,000 g/mol. In a preferred embodiment, the weight average over all molecular weights of all polyalkylene oxides that are contained in the pharmaceutical dosage form is at least 200,000 g/mol. Thus, polyalkylene glycols, if any, are preferably not taken into consideration when determining the weight average molecular weight of polyalkylene oxide (C).
Preferably, the content of the polyalkylene oxide (C) is within the range of from 20 to 99 wt.-%, more preferably 25 to 95 wt.-%, still more preferably 30 to 90 wt.-%, yet more preferably 30 to 85 wt.-%, most preferably 30 to 80 wt.-% and in particular 30 to 75 wt.-%, based on the total weight of the pharmaceutical dosage form. In a preferred embodiment, the content of the -polyalkylene oxide -is at least 20 wt.-%, more preferably at least 25 wt.-%, still more preferably at least 30 wt.-%, yet more preferably at least 35 wt.-% and in particular at least 40 wt.-%.
In a preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 25 20 wt.-%, more preferably 25 15 wt.-%, most preferably 25 10 wt.-%, and in particular 25 5 wt.-%. In another preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 35 20 wt.-%, more preferably 35 15 wt.-%, most preferably 35 10 wt.-%, and in particular 35 5 wt.-%. In still another preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 45 20 wt.-%, more preferably 45 15 wt.-%, most preferably 45 10 wt.-%, and in particular 45 5 wt.-%. In yet another preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 55 20 wt.-%, more prefer-ably 55 15 wt.-%, most preferably 55 10 wt.-%, and in particular 55 5 wt.-%.
In a further preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 65 20 wt.-%, more preferably 65 15 wt.-%, most preferably 65 10 wt.-%, and in particular 65 5 wt.-%. In still a further a preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 75 20 wt.-%, more preferably 75 15 wt.-%, most preferably 75 10 wt.-%, and in particular 75 5 wt.-%. In a still further a preferred embodiment, the overall content of polyalkylene oxide (C) is within the range of 80 15 wt.-%, more preferably 80 10 wt.-%, and most preferably 80 5 wt.-%.
In a preferred embodiment, polyalkylene oxide (C) is homogeneously distributed in the pharmaceutical dosage form according to the invention. Preferably, polyalkylene oxide (C) forms a matrix in which the opioid (A) is embedded. In a particularly preferred embodiment, the opioid (A) and polyalkylene oxide (C) are intimately homogeneously distributed in the pharmaceutical dosage form so that the pharmaceutical dosage form does not contain any segments where either opioid (A) is present in the absence of polyalkylene oxide (C) or where polyalkylene oxide (C) is present in the absence of opioid (A).
When the pharmaceutical dosage form is film coated, the polyalkylene oxide (C) is preferably homogeneously distributed in the core of the pharmaceutical dosage form, i.e.
the film coating preferably does not contain polyalkylene oxide (C). Nonetheless, the film coating as such may of course contain one or more polymers, which however, preferably differ from the polyalkylene oxide (C) contained in the core.
The polyalkylene oxide (C) may be combined with one or more different polymers selected from the group consisting of polyalkylene oxide, preferably polymethylene oxide, polyethy-lene oxide, polypropylene oxide; polyethylene, polypropylene, polyvinyl chloride, polycarbo-nate, polystyrene, polyvinylpyrrolidone, poly(alk)acrylate, poly(hydroxy fatty acids), such as for example poly(3-hydroxybutyrate-co-3-hydroxyvalerate) (Biopol ), poly(hydroxyvaleric acid); polycaprolactone, polyvinyl alcohol, polyesteramide, polyethylene succinate, polylac-tone, polyglycolide, polyurethane, polyamide, polylactide, polyacetal (for example poly-saccharides optionally with modified side chains), polylactide/glycolide, polylactone, poly-glycolide, polyorthoester, polyanhydride, block polymers of polyethylene glycol and polybuty-lene terephthalate (Polyactive ), polyanhydride (Polifeprosan), copolymers thereof, block-copolymers thereof, and mixtures of at least two of the stated polymers, or other polymers with the above characteristics.
Preferably, the molecular weight dispersity M,N/Mõ of polyalkylene oxide (C) is within the range of 2.5 2.0, more preferably 2.5 1.5, still more preferably 2.5 1.0, yet more preferably 2.5 0.8, most preferably 2.5 0.6, and in particular 2.5 0.4.
The polyalkylene oxide (C) preferably has a viscosity at 25 C of 30 to 17,600 cP, more preferably 55 to 17,600 cP, still more preferably 600 to 17,600 cP and most preferably 4,500 to 17,600 cP, measured in a 5 wt.-% aqueous solution using a model RVF
Brookfield viscosimeter (spindle no. 2 / rotational speed 2 rpm); of 400 to 4,000 cP, more preferably 400 to 800 cP or 2,000 to 4,000 cP, measured on a 2 wt.-% aqueous solution using the stated viscosimeter (spindle no. 1 or 3 / rotational speed 10 rpm); or of 1,650 to 10,000 cP, more preferably 1,650 to 5,500 cP, 5,500 to 7,500 cP or 7,500 to 10,000 cP, measured on a 1 wt.-% aqueous solution using the stated viscosimeter (spindle no. 2 / rotational speed 2 rpm).
In a preferred embodiment according to the invention the polyalkylene oxide (C) having a weight average molecular weight of at least 200,000 g/mol is combined with at least one further polymer, preferably but not necessarily also having a weight average molecular weight (Mw) of at least 200,000 g/mol, selected from the group consisting of polyethylene, polypropylene, polyvinyl chloride, polycarbonate, polystyrene, polyacrylate, poly(hydroxy fatty acids), polycaprolactone, polyvinyl alcohol, polyesteramide, polyethylene succinate, poly-lactone, polyglycolide, polyurethane, polyvinylpyrrolidone, polyamide, polylactide, polylactide/
glycolide, polylactone, polyglycolide, polyorthoester, polyanhydride, block polymers of polyethylene glycol and polybutylene terephthalate, polyanhydride, polyacetal, cellulose esters, cellulose ethers and copolymers thereof. Cellulose esters and cellulose ethers are particularly preferred, e.g. methylcelIulose, ethylcellulose, hydroxymethylcelIulose, hydroxy-ethylcellulose, hydroxypropylcellulose hydroxypropylmethylcellulose, ca rboxymethylcel I u lose, and the like.
In a preferred embodiment, said further polymer is neither a polyalkylene oxide nor a poly-alkylene glycol. Nonetheless, the pharmaceutical dosage form may contain polyalkylene glycol, e.g. as plasticizer, but then, the pharmaceutical dosage form preferably is a ternary mixture of polymers: polyalkylene oxide (C) + further polymer + plasticizer.
In a particularly preferred embodiment, said further polymer is a hydrophilic cellulose ester or cellulose ether, preferably hydroxypropylmethylcellulose (HPMC), hydroxypropylcellulose (HPC) or hyd roxyeth ylcel I u lose (HEC), preferably having an average viscosity (preferably measured by capillary viscosimetry or rotational viscosimetry) of 1,000 to 150,000 mPas, more preferably 3,000 to 150,000. In a preferred embodiment, the average viscosity is within the range of 110,000 50,000 mPas, more preferably 110,000 40,000 mPas, still more preferably 110,000 30,000 mPas, most preferably 110,000 20,000 mPas, and in particular 100,000 10,000 mPas.
In a preferred embodiment the relative weight ratio of said polyalkylene oxide (C) and said further polymer is within the range of from 20:1 to 1:20, more preferably 10:1 to 1:10, still more preferably 7:1 to 1:5, yet more preferably 5:1 to 1:1, most preferably 4:1 to 1,5:1 and in particular 3:1 to 2:1. In a preferred embodiment, the relative weight ratio of said polyalkylene oxide (C) and said further polymer is within the range of from 10:1 to 5:1, more preferably 8:1 to 5:1, most preferably 7:1 to 5:1.
Preferably, the content of said further polymer amounts to 0.5 to 25 wt.-%, more preferably 1.0 to 20 wt.-%, still more preferably 2.0 to 22.5 wt.-%, yet more preferably 3.0 to 20 wt.-%
and most preferably 4.0 to 17.5 wt.-% and in particular 5.0 to 15 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the further polymer is a cellulose ester or cellulose ether, prefer-ably HPMC, having a content within the range of 10 8 wt.-%, more preferably 10
6 wt.-%, still more preferably 10 5 wt.-%, yet more preferably 10 4 wt.-%, most preferably 10 3 wt.-%, and in particular 10 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
In another preferred embodiment, the further polymer is a cellulose ester or cellulose ether, preferably HPMC, having a content within the range of 14 8 wt.-%, more preferably 14 6 wt.-%, still more preferably 14 5 wt.-%, yet more preferably 14 4 wt.-%, most preferably 14 3 wt.-%, and in particular 14 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
All polymers are preferably employed as powders. They can be soluble in water.
Besides the opioid (A), the acid (B) and polyalkylene oxide (C) the pharmaceutical dosage form according to the invention may contain further constituents, such as conventional pharmaceutical excipients.
Preferably, the pharmaceutical dosage form comprises an antioxidant. Suitable antioxidants include ascorbic acid, a-tocopherol (vitamin E), butylhydroxyanisol, butylhydroxytoluene, salts of ascorbic acid (vitamin C), ascorbylic palmitate, monothioglycerine, coniferyl benzoate, nordihydroguajaretic acid, gallus acid esters, phosphoric acid, and the derivatives thereof, such as vitamin E-succinate or vitamin E-palmitate and/or sodium bisulphite, more preferably butyihydroxytoluene (BHT) or butylhydroxyanisol (BHA) and/or a-tocopherol.
Preferably, the content of the antioxidant is within the range of from 0.001 to 5.0 wt.-%, more preferably 0.002 to 2.5 wt.-%, more preferably 0.003 to 1.5 wt.-%, still more preferably 0.005 to 1.0 wt.-%, yet more preferably 0.01 to 0.5 wt.-%, most preferably 0.05 to 0.4 wt.-% and in particular 0.1 to 0.3 wt.-%, based on the total weight of the pharmaceutical dosage form.
A particularly preferred antioxidant is a-tocopherol. It has been surprisingly found that a-tocopherol stabilizes polyalkylene oxide and simultaneously destabilizes certain opioids (A), such as oxymorphone. Thus, in a preferred embodiment, the content of a-tocopherol is balanced between a sufficient stability of the polyalkylene oxide on the one hand and a sufficient stability of the opioid (A) on the other hand.
In a preferred embodiment, the content of a-tocopherol is within the range of 0.2 0.18 wt.-%, more preferably 0.2 0.15 wt.-%, still more preferably 0.2 0.12 wt.-%, yet more preferably 0.2 0.09 wt.-%, most preferably 0.2 0.06 wt.-%, and in particular 0.2 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the relative weight ratio of the acid (B), preferably citric acid, and the antioxidant, preferably a-tocopherol, is within the range of from 10:1 to 1:10, more preferably 8:1 to 1:8, still more preferably 6:1 to 1:6, yet more preferably 5:1 to 1:4, most preferably 4:1 to 1:3 and in particular 3:1 to 1:2.
The pharmaceutical dosage form according to the invention may also contain a natural, semi-synthetic or synthetic wax. Waxes with a softening point of at least 50 C, more preferably 60 C are preferred. Carnauba wax and beeswax are particularly preferred, especially carnauba wax.
Preferably, the release profile of the opioid (A) is matrix-retarded.
Preferably, the opioid (A) is embedded in a matrix comprising the polyalkylene oxide, said matrix controlling the release of the opioid (A) from the pharmaceutical dosage form.
Physiologically acceptable materials which are known to the person skilled in the art may be used as supplementary matrix materials. Polymers, particularly preferably cellulose ethers, cellulose esters and/or acrylic resins are preferably used as hydrophilic matrix materials.
Ethylcellulose, hydroxypropylmethylcellulose, hyd roxypro pylcel I u lose, hydroxymethylcellu-lose, hydroxyethylcellulose, poly(meth)acrylic acid and/or the derivatives thereof, such as the salts, amides or esters thereof are very particularly preferably used as matrix materials.
Matrix materials prepared from hydrophobic materials, such as hydrophobic polymers, waxes, fats, long-chain fatty acids, fatty alcohols or corresponding esters or ethers or mixtures thereof are also preferred. Mono- or diglycerides of C12-C30 fatty acids and/or C12-C30 fatty alcohols and/or waxes or mixtures thereof are particularly preferably used as hydrophobic materials. It is also possible to use mixtures of the above-stated hydrophilic and hydrophobic materials as matrix materials.
Preferably, the relative weight ratio of the polyalkylene oxide to the opioid (A) is at least 0.5:1, more preferably at least 1:1, at least 2:1, at least 3:1, at least 4:1, at least 5:1, at least 6:1, at least 7:1, at least 8:1 or at least 9:1; still more preferably at least 10:1 or at least 15:1, yet more preferably at least 20:1, most preferably at least 30:1 and in particular at least 40:1.
In a preferred embodiment, the relative weight ratio of the polyalkylene oxide to the opioid (A) is within the range of from 3:1 to 50:1, more preferably 3:1 to 40:1 and in particular 3:1 to 30:1.
The pharmaceutical dosage form according to the invention preferably contains a plasticizer.
The plasticizer improves the processability of the polyalkylene oxide. A
preferred plasticizer is polyalkylene glycol, like polyethylene glycol, triacetin, fatty acids, fatty acid esters, waxes and/or microcrystalline waxes. Particularly preferred plasticizers are polyethylene glycols, such as PEG 6000.
Preferably, the content of the plasticizer is within the range of from 0.1 to 25 wt.-%, more preferably 0.5 to 22.5 wt.-%, still more preferably 1.0 to 20 wt.-%, yet more preferably 2.5 to 17.5 wt.-%, most preferably 5.0 to 15 wt.-% and in particular 7.5 to 12.5 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the plasticizer is a polyalkylene glycol having a content within the range of 10 8 wt.-%, more preferably 10 6 wt.-%, still more preferably 10 5 wt.-%, yet more preferably 10 4 wt.-%, most preferably 10 3 wt.-%, and in particular 10 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
In another preferred embodiment, the plasticizer is a polyalkylene glycol having a content within the range of 15 8 wt.-%, more preferably 15 6 wt.-%, still more preferably 15 5 wt.-%, yet more preferably 15 4 wt.-%, most preferably 15 3 wt.-%, and in particular 15 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the relative weight ratio of the polyalkylene oxide to the polyalkylene glycol is within the range of 4.2 2 : 1, more preferably 4.2 1.5 : 1, still more preferably 4.2 1 : 1, yet more preferably 4.2 0.5 : 1, most preferably 4.2 0.2 : 1, and in particular 4.2 0.1 : 1. This ratio satisfies the requirements of relative high polyalkylene oxide content and good extrudability.
When manufacturing the dosage forms from slices that are obtained by cutting the extrudate strand, the weight of the slices determines the weight of the resulting dosage form.
Pronounced variation in weight of these slices results in an accordant weight deviation of dosage forms from the target weight. The weight variation of slices depends strongly on the surface properties of the extrudate strand. A strand with a thoroughly smooth surface allows the generation of slices exhibiting a low weight variation. In contrast, a wavy or shark skinning strand results in slices exhibiting a higher weight variation thereby increasing the number of rejects.
It has now been surprisingly found that the surface properties of the extrudate strand can be triggered by the polyalkylene oxide : polyalkylene glycol weight ratio.
Preferred compositions X, to X32 of the pharmaceutical dosage form according to the invention are summarized in the tables here below:
wt.% X, X2 X3 X4 o ioid (A) (e.g. ox mo hone HCI) 1.50 1.25 1.50 1.00 1.50 0.75 1.50 0.50 acid (B) (e.g. citric acid) 0.5 0.30 0.5 0.25 0.5 0.20 0.5 0.15 of alk lene oxide (C) 77 22 77 20 77 15 77 10 cellulose ester or ether (e.g. HPMC) 12 10 12 7.5 12 5 12 2.5 -plasticizer (e.g. PEG) 10 7.5 10 5 10 2.5 10 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.% X5 X6 X7 X8 o ioid (A) (e.g. ox mo hone HCI) 2.33 1.25 2.33 1.00 2.33 0.75 2.33 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 of alk lene oxide (C) 70 25 70 20 70 15 70 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 -plasticizer (e.g. PEG) 16.6 7.5 16.6 5 16.6 2.5 16.6 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.% X9 X10 X11 X12 opioid (A) (e.g. ox mo hone HCI) 3.50 1.25 3.50 1.00 3.50 0.75 3.50 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 of alk lene oxide (C) 69 30 69 20 69 15 69 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 16.4 7.5 16.4 5 16.4 2.5 16.4 1.0 antioxidant (e.g. a-toco herol 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.% X13 X14 X15 X16 opioid (A) (e.g. ox mo hone HCI) 4.65 1.25 4.65 1.00 4.65 0.75 4.65 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 68 30 68 20 68 15 68 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 16.2 7.5 16.2 5 16.2 2.5 16.2 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 opioid (A) (e.g. ox mo hone HCI) 6.98 1.25 6.98 1.00 6.98 0.75 6.98 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 of alk lene oxide (C) 66 30 66 20 66 15 66 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 15.8 7.5 15.8 5 15.8 2.5 15.8 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.-% X21 X22 X23 X24 opioid (A) (e.g. ox mo hone HCI) 9.30 1.25 9.30 1.00 9.30 0.75 9.30 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 64 30 64 20 64 15 64 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 15.3 7.5 15.3 5 15.3 2.5 15.3 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.-% X25 X26 X27 X28 opioid (A) (e.g. ox mo hone HCI 13.95 1.25 13.95 1.00 13.95 0.75 13.95 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 60 30 60 20 60 15 60 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 13.9 7.5 13.9 5 13.9 2.5 13.9 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.-% X29 X3o X31 X32 opioid (A) (e.g. ox mo hone HCI) 18.60 1.25 18.60 1.00 18.60 0.75 18.60 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 57 30 57 20 57 15 57 10 cellulose ester or ether (e.g. HPMC 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 13.6 7.5 13.6 5 13.6 2.5 13.6 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 In a preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 100 75 mg, more preferably 100 50 mg, most preferably 100 25 mg. In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 200 75 mg, more preferably 200 50 mg, most preferably 200 25 mg. In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 250 75 mg, more preferably 250 50 mg, most preferably 250 25 mg. In still another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 300 75 mg, more preferably 300 50 mg, most preferably 300 25 mg. In yet another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 400 75 mg, more preferably 400 50 mg, most preferably 400 25 mg.
In a preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 500 250 mg, more preferably 500 200 mg, most preferably 500 150 mg.
In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 750 250 mg, more preferably 750 200 mg, most preferably 750 150 mg. In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 1000 250 mg, more preferably 1000 200 mg, most preferably 1000 150 mg. In still another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 1250 250 mg, more preferably 1250 200 mg, most preferably 1250 150 mg.
In a preferred embodiment, the pharmaceutical dosage form according to the invention has an overall density within the range of 1.19 0.30 g/cm3, more preferably 1.19 0.25 g/cm3, still more preferably 1.19 0.20 g/cm3, yet more preferably 1.19 0.15 g/cm3, most preferably 1.19 0.10 g/cm3, and in particular 1.19 0.05 g/cm3. Preferably, the overall density of the pharmaceutical dosage form according to the invention is 1.17 0.02 g/cm3, 1.19 0.02 g/cm3 or 1.21 0.02 g/cm3. Methods for measuring the density of a dosage form are known to a person skilled in the art. The overall density of a dosage form can for example be determined by means of the mercury porosimetry method or the helium pycnometer method as described in Ph. Eur.
Preferably, the pharmaceutical dosage form according to the invention is adapted for oral administration. It is also possible, however, to administer the pharmaceutical dosage form via different routes and thus, the pharmaceutical dosage form may alternatively be adapted for buccal, lingual, rectal or vaginal administration. Implants are also possible.
In a preferred embodiment, the pharmaceutical dosage form according to the invention is adapted for administration once daily. In another preferred embodiment, the pharmaceutical dosage form according to the invention is adapted for administration twice daily. In still another preferred embodiment, the pharmaceutical dosage form according to the invention is adapted for administration thrice daily.
For the purpose of the specification, "twice daily" means equal or nearly equal time intervals, i.e., about every 12 hours, or different time intervals, e.g., 8 and 16 hours or 10 and 14 hours, between the individual administrations.
For the purpose of the specification, "thrice daily" means equal or nearly equal time intervals, i.e., about every 8 hours, or different time intervals, e.g., 6, 6 and 12 hours; or 7, 7 and 10 hours, between the individual administrations.
Preferably, the pharmaceutical dosage form according to the invention causes an at least partially delayed or prolonged release of opioid (A).
Controlled or prologned release is understood according to the invention preferably to mean a release profile in which the opioid (A) is released over a relatively long period with reduced intake frequency with the purpose of extended therapeutic action. Preferably, the meaning of the term "prolonged release" is in accordance with the European guideline on the nomen-clature of the release profile of pharmaceutical dosage forms (CHMP). This is achieved in particular with peroral administration. The expression "at least partially delayed or prolonged release" covers according to the invention any pharmaceutical dosage forms which ensure modified release of the opioids (A) contained therein. The pharmaceutical dosage forms preferably comprise coated or uncoated pharmaceutical dosage forms, which are produced with specific auxiliary substances, by particular processes or by a combination of the two possible options in order purposefully to change the release rate or location of release.
In the case of the pharmaceutical dosage forms according to the invention, the release time profile of a controlled release form may be modified e.g. as follows: extended release, repeat action release, prolonged release and sustained release.
For the purpose of the specification "controlled release" preferably means a product in which the release of active compound over time is controlled by the type and composition of the formulation. For the purpose of the specification "extended release"
preferably means a product in which the release of active compound is delayed for a finite lag time, after which release is unhindered. For the purpose of the specification "repeat action release" preferably means a product in which a first portion of active compound is released initially, followed by at least one further portion of active compound being released subsequently.
For the purpose of the specification "prolonged release" preferably means a product in which the rate of release of active compound from the formulation after administration has been reduced over time, in order to maintain therapeutic activity, to reduce toxic effects, or for some other therapeutic purpose. For the purpose of the specification "sustained release"
preferably means a way of formulating a medicine so that it is released into the body steadily, over a long period of time, thus reducing the dosing frequency. For further details, reference may be made, for example, to K.H. Bauer, Lehrbuch der Pharmazeutischen Technologie, 6th edition, WVG Stuttgart, 1999; and Eur. Ph.
The pharmaceutical dosage form according to the invention may comprise one or more opioids (A) at least in part in a further controlled release form, wherein controlled release may be achieved with the assistance of conventional materials and processes known to the person skilled in the art, for example by embedding the substance in a controlled release matrix or by applying one or more controlled release coatings. Substance release must, however, be controlled such that addition of delayed-release materials does not impair the necessary breaking strength. Controlled release from the pharmaceutical dosage form according to the invention is preferably achieved by embedding the substance in a matrix.
Preferably, polyalkylene oxide (C) serves as such a matrix. The auxiliary substances acting as matrix materials control release. Matrix materials may, for example, be hydrophilic, gel-forming materials, from which release proceeds mainly by diffusion, or hydrophobic materials, from which release proceeds mainly by diffusion from the pores in the matrix.
Preferably, the release profile is substantially matrix controlled, preferably by embedding opioid (A) in a matrix comprising polyalkylene oxide (C) and optionally, further matrix materials. Preferably, the release profile is not osmotically driven.
Preferably, release kinetics is not zero order.
Preferably, under physiological conditions the pharmaceutical dosage form according to the invention has released after 30 minutes 0.1 to 75%, after 240 minutes 0.5 to 95%, after 480 minutes 1.0 to 100% and after 720 minutes 2:5 to 100% of the opioid (A).
Further preferred release profiles R, to R6 are summarized in the table here below [all data in wt.-% of released opioid (A)]:
time R, R2 R3 R4 R5 R6 60 min 0-30 0-50 0-50 15-25 20-30 20-50 120 min 0-40 0-75 0-75 25-40 35-50 40-75 240 min 3-55 3-95 10-95 40-70 55-75 60-95 480 min 10-65 10-100 35-100 60-90 80-95 80-100 720 min 20-75 20-100 55-100 70-100 90-100 90-100 960 min 30-88 30-100 70-100 >80 95-100 1440 min 50-100 50-100 >90 2160 min >80 >80 Further preferred release profiles R, to R6 are summarized in the table here below [all data in wt.-% of released opioid (A)]:
time R7 R8 R9 Rip R11 R12 30 min 17.5 7.5 17.5 6.5 17.5 5.5 17.5 4.5 17.5 3.5 17.5 2.5 60 min 27.0 8.0 27.0 7.0 27.0 6.0 27.0 5.0 27.0 4.0 27.0 3.0 120 min 41.5 9.5 41.5 8.5 41.5 7.5 41.5 6.5 41.5 5.5 41.5 4.5 240 min 64.5 12.5 64.5 11.5 64.5 10.5 64.5 9.5 64.5 8.5 64.5 7.5 480 min 88.0 12.0 88.0 11.0 88.0 10.0 88.0 9.0 88.0 8.0 88.0 7.0 720 min 96.0 9.0 96.0 8.0 96.0 7.0 96.0 6.0 96.0 5.0 96.0 4.0 840 min 97.5 7.5 97.5 6.5 97.5 5.5 97.5 4.5 97.5 3.5 97.5 2.5 Preferably, the release profile of the pharmaceutical dosage form according to the present invention is stable upon storage, preferably upon storage at elevated temperature, e.g. 37 C, for 3 months in sealed containers. In this regard "stable" means that when comparing the initial release profile with the release profile after storage, at any given time point the release profiles deviate from one another by not more than 20%, more preferably not more than 15%, still more preferably not more than 10%, yet more preferably not more than 7.5%, most preferably not more than 5.0% and in particular not more than 2.5%.
Preferably, under in vitro conditions the pharmaceutical dosage form has released after 0.5 h 1.0 to 35 wt.-%, after 1 h 5.0 to 45 wt.-%, after 2 h 10 to 60 wt.-%, after 4 hat least 15 wt.-%, after 6 h at least 20 wt.-%, after 8 h at least 25 wt.-% and after 12 h at least 30 wt.-% of the opioid (A) that was originally contained in the pharmaceutical dosage form.
Suitable in vitro conditions are known to the skilled artisan. In this regard it can be referred to, e.g., the Eur. Ph. Preferably, the release profile is measured under the following conditions: Paddle apparatus equipped with sinker, 50 rpm, 37 5 C, 900 mL
simulated intestinal fluid pH 6.8 (phosphate buffer) or pH 4.5. In a preferred embodiment, to rotational speed of the paddle is increased-to 100 rpm.
In a preferred embodiment, after preferably oral administration of the pharmaceutical dosage form according to the invention, in vivo the average peak plasma level (Cmax) is on average reached after tmax 4.0 2.5 h, more preferably after tmax 4.0 2.0 h, still more preferably after tmax 4.0 1.5 h, most preferably after tmax 4.0 1.0 h and in particular after tmax 4.0 0.5 h. In another preferred embodiment, after preferably oral administration of the pharmaceutical dosage form according to the invention, in vivo the average peak plasma level (Cmax) is on average reached after tmax 5.0 2.5 h, more preferably after tmax 5.0 2.0 h, still more preferably after tmax 5.0 1.5 h, most preferably after tmax 5.0 1.0 h and in particular after tmax 5.0 0.5 h. In still another preferred embodiment, after preferably oral administration of the pharmaceutical dosage form according to the invention, in vivo the average peak plasma level (Cmax) is on average reached after tmax 6.0 2.5 h, more preferably after tmax 6.0 2.0 h, still more preferably after tmax 6.0 1.5 h, most preferably after tmax 6.0 1.0 h and in particular after tmax 6.0 0.5 h.
In a preferred embodiment, the average value for t12 after preferably oral administration of the pharmaceutical dosage form according to the invention in vivo is 4.0 2.5 h, more preferably 4.0 2.0 h, still more preferably 4.0 1.5 h, most preferably 4.0 1.0 h, and in particular 4.0 0.5 h. In another preferred embodiment, the average value for t12 after preferably oral administration of the pharmaceutical dosage form according to the invention in vivo is preferably 5.0 2.5 h, more preferably 5.0 2.0 h, still more preferably 5.0 1.5 h, most preferably 5.0 1.0 h, and in particular 5.0 0.5 h. In still another preferred embodiment, the average value for t12 after preferably oral administration of the pharmaceutical dosage form according to the invention in vivo is preferably 6.0 2.5 h, more preferably 6.0 2.0 h, still more preferably 6.0 1.5 h, most preferably 6.0 1.0 h, and in particular 6.0 0.5 h.
Preferably, the pharmaceutical dosage form according to the invention contains a coating, preferably a film-coating. Suitable coating materials are known to the skilled person. Suitable coating materials are commercially available, e.g. under the trademarks Opadry and Eudragit .
Examples of suitable materials include cellulose esters and cellulose ethers, such as methyl-cellulose (MC), hydroxypropylmethylcellulose (HPMC), hyd roxypropylcel I u lose (HPC), hyd roxyethylcel I u lose (HEC), sodium carboxymethylcellulose (Na-CMC), ethylcellulose (EC), cellulose acetate phthalate (CAP), hydroxypropylmethylcellulose phthalate (HPMCP);
poly(meth)acrylates, such as aminoalkylmethacrylate copolymers, ethylacrylate methyl-methacrylate copolymers, methacrylic acid methylmethacrylate copolymers, methacrylic acid methylmethacrylate copolymers; vinyl polymers, such as polyvinylpyrrolidone, polyvinyl-acetatephtha late, polyvinyl alcohol, polyvinylacetate; and natural film formers, such as shellack.
In a particularly preferred embodiment, the coating is water-soluble. In a preferred embodiment, the coating is based on polyvinyl alcohol, such as polyvinyl alcohol-part.
hydrolyzed, and may additionally contain polyethylene glycol, such as macrogol 3350, and/or pigments. In another preferred embodiment, the coating is based on hydroxypropylmethyl-cellulose, preferably hypromellose type 2910 having a viscosity of 3 to 15 mPas.
The coating of the pharmaceutical dosage form can increase its storage stability.
The coating can be resistant to gastric juices and dissolve as a function of the pH value of the release environment. By means of this coating, it is possible to ensure that the pharmaceutical dosage form according to the invention passes through the stomach undissolved and the active compound is only released in the intestines. The coating which is resistant to gastric juices preferably dissolves at a pH value of between 5 and 7.5.
Corresponding materials and methods for the delayed release of active compounds and for the application of coatings which are resistant to gastric juices are known to the person skilled in the art, for example from "Coated Pharmaceutical dosage forms -Fundamentals, Manufacturing Techniques, Biopharmaceutical Aspects, Test Methods and Raw Materials"
by Kurt H. Bauer, K. Lehmann, Hermann P. Osterwald, Rothgang, Gerhart, 1st edition, 1998, Medpharm Scientific Publishers.
In a preferred embodiment, the pharmaceutical dosage form according to the invention contains no substances which irritate the nasal passages and/or pharynx, i.e.
substances which, when administered via the nasal passages and/or pharynx, bring about a physical reaction which is either so unpleasant for the patient that he/she does not wish to or cannot continue administration, for example burning, or physiologically counteracts taking of the corresponding active compound, for example due to increased nasal secretion or sneezing.
Further examples of substances which irritate the nasal passages and/or pharynx are those which cause burning, itching, urge to sneeze, increased formation of secretions or a combi-nation of at least two of these stimuli. Corresponding substances and the quantities thereof which are conventionally to be used are known to the person skilled in the art. Some of the substances which irritate the nasal passages and/or pharynx are accordingly based on one or more constituents or one or more plant parts of a hot substance drug.
Corresponding hot substance drugs are known per se to the person skilled in the art and are described, for example, in "Pharmazeutische Biologie - Drogen and ihre Inhaltsstoffe" by Prof. Dr. Hildebert Wagner, 2nd., revised edition, Gustav Fischer Verlag, Stuttgart-New York, 1982, pages 82 et seq.. The corresponding description is hereby introduced as a reference and is deemed to be part of the disclosure.
The pharmaceutical dosage form according to the invention furthermore preferably contains no antagonists for the opioid (A), preferably no antagonists against psychotropic substances, in particular no antagonists against opioids (A). Antagonists suitable for a given opioid (A) are known to the person skilled in the art and may be present as such or in the form of corresponding derivatives, in particular esters or ethers, or in each case in the form of corresponding physiologically acceptable compounds, in particular in the form of the salts or solvates thereof. The pharmaceutical dosage form according to the invention preferably contains no antagonists selected from among the group comprising naloxone, naltrexone, nalmefene, nalide, nalmexone, nalorphine or naluphine, in each case optionally in the form of a corresponding physiologically acceptable compound, in particular in the form of a base, a salt or solvate; and no neuroleptics, for example a compound selected from among the group comprising haloperidol, promethacine, fluphenazine, perphenazine, levomepromazine, thiori-dazine, perazine, chlorpromazine, chlorprothixine, zuclopenthixol, flupentixol, prothipendyl, zotepine, benperidol, pipamperone, melperone and bromperidol.
The pharmaceutical dosage form according to the invention furthermore preferably contains no emetic. Emetics are known to the person skilled in the art and may be present as such or in the form of corresponding derivatives, in particular esters or ethers, or in each case in the form of corresponding physiologically acceptable compounds, in particular in the form of the salts or solvates thereof. The pharmaceutical dosage form according to the invention preferably contains no emetic based on one or more constituents of ipecacuanha (ipecac) root, for example based on the constituent emetine, as are, for example, described in "Pharmazeutische Biologie - Drogen and ihre Inhaltsstoffe" by Prof. Dr.
Hildebert Wagner, 2nd, revised edition, Gustav Fischer Verlag, Stuttgart, New York, 1982. The corresponding literature description is hereby introduced as a reference and is deemed to be part of the disclosure. The pharmaceutical dosage form according to the invention preferably also contains no apomorphine as an emetic.
Finally, the pharmaceutical dosage form according to the invention preferably also contains no bitter substance. Bitter substances and the quantities effective for use may be found in US-2003/0064099 Al, the -corresponding disclosure of which should be deemed to be the disclosure of the present application and is hereby introduced as a reference.
Examples of bitter substances are aromatic oils, such as peppermint oil, eucalyptus oil, bitter almond oil, menthol, fruit aroma substances, aroma substances from lemons, oranges, limes, grapefruit or mixtures thereof, and/or denatonium benzoate.
The pharmaceutical dosage form according to the invention accordingly preferably contains neither substances which irritate the nasal passages and/or pharynx, nor antagonists for the opioid (A), nor emetics, nor bitter substances.
The pharmaceutical dosage form according to the invention is preferably adapted for oral administration.
Typically, the pharmaceutical dosage form according to the invention assumes the form of a tablet. Preferably, the pharmaceutical dosage form is neither in film form, nor multi-particulate.
The pharmaceutical dosage form according to the invention is preferably tamper-resistant.
Preferably, tamper-resistance is achieved based on the mechanical properties of the pharmaceutical dosage form so that comminution is avoided or at least substantially impeded. According to the invention, the term comminution means the pulverization of the pharmaceutical dosage form using conventional means usually available to an abuser, for example a pestle and mortar, a hammer, a mallet or other conventional means for pulverizing under the action of force. Thus, tamper-resistance preferably means that pulverization of the pharmaceutical dosage form using conventional means is avoided or at least substantially impeded.
Preferably, the mechanical properties of the pharmaceutical dosage form according to the invention, particularly its breaking strength, substantially rely on the presence and spatial distribution of polyalkylene oxide (C), although its mere presence does typically not suffice in order to achieve said properties. The advantageous mechanical properties of the pharma-ceutical dosage form according to the invention may not automatically be achieved by simply processing opioid (A), acid (B), polyalkylene oxide (C), and optionally further excipients by means of conventional methods for the preparation of pharmaceutical dosage forms. In fact, usually suitable apparatuses must be selected for the preparation and critical processing parameters must be adjusted, particularly pressure/force, temperature and time. Thus, even if conventional apparatuses are used, the process protocols usually must be adapted in order to meet the required criteria.
The pharmaceutical dosage form according to the invention has a breaking strength of at least 300 N, preferably at least 400 N, more preferably at least 500 N, still more preferably at least 750 N, yet more preferably at least 1000 N, most preferably at least 1250 N and in particular at least 1500 N.
The "breaking strength" (resistance to crushing) of a pharmaceutical dosage form is known to the skilled person. In this regard it can be referred to, e.g., W.A. Ritschel, Die Tablette, 2.
Auflage, Editio Cantor Verlag Aulendorf, 2002; H Liebermann et al., Pharmaceutical dosage forms: Tablets, Vol. 2, Informa Healthcare; 2 edition, 1990; and Encyclopedia of Pharma-ceutical Technology, Informa Healthcare; 1 edition.
For the purpose of the specification, the breaking strength is preferably defined as the amount of force that is necessary in order to fracture the pharmaceutical dosage form breaking force). Therefore, for the purpose of the specification the pharmaceutical dosage form does preferably not exhibit the desired breaking strength when it breaks, i.e., is fractured into at least two independent parts that are separated from one another. In another preferred embodiment, however, the pharmaceutical dosage form is regarded as being broken if the force decreases by 25% (threshold value) of the highest force measured during the measurement (see below).
The pharmaceutical dosage forms according to the invention are distinguished from conventional pharmaceutical dosage forms in that, due to their breaking strength, they cannot be pulverized by the application of force with conventional means, such as for example a pestle and mortar, a hammer, a mallet or other usual means for pulverization, in particular devices developed for this purpose (tablet crushers). In this regard "pulverization"
means crumbling into small particles that would immediately release the pharmacologically active compound (A) in a suitable medium. Avoidance of pulverization virtually rules out oral or parenteral, in particular intravenous or nasal abuse.
Conventional tablets typically have a breaking strength well below 200 N in any direction of extension. The breaking strength of conventional round tablets may be estimated according to the following empirical formula: Breaking Strength [in N] = 10 x Diameter Of The Tablet [in mm]. Thus, according to said empirical formula, a round tablet having a breaking strength of at least 300 N would require a diameter of at least 30 mm). Such a tablet, however, could not be swallowed. The above empirical formula preferably does not apply to the pharmaceutical dosage forms of the invention, which are not conventional but rather special.
Further, the actual mean chewing force is about 220 N (cf., e.g., P.A.
Proeschel et al., J Dent Res, 2002, 81(7), 464-468). This means that conventional tablets having a breaking strength well below 200 N may be crushed upon spontaneous chewing, whereas the pharmaceutical dosage forms according to the invention may not.
Still further, when applying a gravitational acceleration of about 9.81 m/s2, 300 N correspond to a gravitational force of more than 30 kg, i.e. the pharmaceutical dosage forms according to the invention can preferably withstand a weight of more than 30 kg without being pulverised.
Methods for measuring the breaking strength of a pharmaceutical dosage form are known to the skilled artisan. Suitable devices are commercially available.
For example, the breaking strength (resistance to crushing) can be measured in accordance with the Eur. Ph. 5.0, 2.9.8 or 6.0, 2.09.08 "Resistance to Crushing of Tablets". The test is intended to determine, under defined conditions, the resistance to crushing of tablets, measured by the force needed to disrupt them by crushing. The apparatus consists of 2 jaws facing each other, one of which moves towards the other. The flat surfaces of the jaws are perpendicular to the direction of movement. The crushing surfaces of the jaws are flat and larger than the zone of contact with the tablet. The apparatus is calibrated using a system with a precision of 1 Newton. The tablet is placed between the jaws, taking into account, where applicable, the shape, the break-mark and the inscription; for each measurement the tablet is oriented in the same way with respect to the direction of application of the force (and the direction of extension in which the breaking strength is to be measured).
The measurement is carried out on 10 tablets, taking care that all fragments of tablets have been removed before each determination. The result is expressed as the mean, minimum and maximum values of the forces measured, all expressed in Newton.
A similar description of the breaking strength (breaking force) can be found in the USP. The breaking strength can alternatively be measured in accordance with the method described therein where it is stated that the breaking strength is the force required to cause a tablet to fail (i.e., break) in a specific plane. The tablets are generally placed between two platens, one of which moves to apply sufficient force to the tablet to cause fracture.
For conventional, round (circular cross-section) tablets, loading occurs across their diameter (sometimes referred to as diametral loading), and fracture occurs in the plane. The breaking force of tablets is commonly called- hardness in the pharmaceutical literature;
however, the use of this term is misleading. In material science, the term hardness refers to the resistance of a surface to penetration or indentation by a small probe. The term crushing strength is also frequently used to describe the resistance of tablets to the application of a compressive load.
Although this term describes the true nature of the test more accurately than does hardness, it implies that tablets are actually crushed during the test, which is often not the case.
Alternatively, the breaking strength (resistance to crushing) can be measured in accordance with WO 2005/ 016313, WO 2005/016314, and WO 2006/082099, which can be regarded as a modification of the method described in the Eur. Ph. The apparatus used for the measurement is preferably a "Zwick Z 2.5" materials tester, Finax = 2.5 kN
with a maximum draw of 1150 mm, which should be set up with one column and one spindle, a clearance behind of 100 mm and a test speed adjustable between 0.1 and 800 mm/min together with testControl software. Measurement is performed using a pressure piston with screw-in inserts and a cylinder (diameter 10 mm), a force transducer, Finax= 1 kN, diameter = 8 mm, class 0.5 from 10 N, class 1 from 2 N to ISO 7500-1, with manufacturer's test certificate M
according to DIN 55350-18 (Zwick gross force Finaz = 1.45 kN) (all apparatus from Zwick GmbH & Co. KG, Ulm, Germany) with Order No BTC-FR 2.5 TH. D09 for the tester, Order No BTC-LC 0050N. P01 for the force transducer, Order No BO 70000 S06 for the centring device.
In a preferred embodiment of the invention, the breaking strength is measured by means of a breaking strength tester e.g. Sotax , type HT100 or type HT1 (Allschwil, Switzerland). Both, the Sotax HT100 and the Sotax HT1 can measure the breaking strength according to two different measurement principles: constant speed (where the test jaw is moved at a constant speed adjustable from 5-200 mm/min) or constant force (where the test jaw increases force linearly adjustable from 5-100 N/sec). In principle, both measurement principles are suitable for measuring the breaking strength of the pharmaceutical dosage form according to the invention. Preferably, the breaking strength is measured at constant speed, preferably at a constant speed of 120 mm/min.
In a preferred embodiment, the pharmaceutical dosage form is regarded as being broken if it is fractured into at least two separate pieces.
The pharmaceutical dosage form according to the invention preferably exhibits mechanical strength over a wide temperature range, in addition to the breaking strength (resistance to crushing) optionally also sufficient hardness, impact resistance, -impact elasticity, tensile strength and/or modulus of elasticity, optionally also at low temperatures (e.g. below -24 C, below -40 C or in liquid nitrogen), for it to be virtually impossible to pulverize by spontaneous chewing, grinding in a mortar, pounding, etc. Thus, preferably, the comparatively high breaking strength of the pharmaceutical dosage form according to the invention is main-tained even at low or very low temperatures, e.g., when the pharmaceutical dosage form is initially chilled to increase its brittleness, for example to temperatures below -25 C, below -40 C or even in liquid nitrogen.
The pharmaceutical dosage form according to the invention is characterized by a certain degree of breaking strength. This does not mean that the pharmaceutical dosage form must also exhibit a certain degree of hardness. Hardness and breaking strength are different physical properties. Therefore, the tamper resistance of the pharmaceutical dosage form does not necessarily depend on the hardness of the pharmaceutical dosage form.
For instance, due to its breaking strength, impact strength, elasticity modulus and tensile strength, respectively, the pharmaceutical dosage form can preferably be deformed, e.g.
plastically, when exerting an external force, for example using a hammer, but cannot be pulverized, i.e., crumbled into a high number of fragments. In other words, the pharmaceutical dosage form according to the invention is characterized by a certain degree of breaking strength, but not necessarily also by a certain degree of form stability.
Therefore, in the meaning of the specification, a pharmaceutical dosage form that is deformed when being exposed to a force in a particular direction of extension but that does not break (plastic deformation or plastic flow) is preferably to be regarded as having the desired breaking strength in said direction of extension.
A particularly preferred embodiment of the invention relates to a tamper-resistant pharmaceutical dosage form having a breaking strength of at least 300 N and being thermoformed by hot-melt extrusion, said pharmaceutical dosage form comprising - an opioid (A) selected from the group consisting of oxymorphone, oxycodone, hydromor-phone, and the physiologically acceptable salts thereof;
- a free physiologically acceptable multicarboxylic acid (B), preferably citric acid, wherein the content of the acid (B) is within the range of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form;
an antioxidant, wherein the content of the antioxidant, preferably a-tocopherol, is within the range of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form; and a polyalkylene oxide (C) having a weight average molecular weight MW of at least 200,000 g/mol;
wherein - the opioid (A) is embedded in a matrix comprising the polyalkylene oxide (C), said matrix controlling the release of the opioid (A) from the pharmaceutical dosage form;
and - after storage for 4 weeks at 40 C and 75% rel. humidity, the content of opioid (A) amounts to at least 98.0% of its original content before storage.
The pharmaceutical dosage form according to the invention may be produced by different processes, the particularly preferred of which are explained in greater detail below. Several suitable processes have already been described in the prior art. In this regard it can be referred to, e.g., WO 2005/ 016313, WO 2005/016314, WO 2005/063214, WO
2005/102286, WO 2006/002883, WO 2006/002884, WO 2006/002886, WO 2006/082097, and WO
2006/082099.
The present invention also relates to pharmaceutical dosage forms that are obtainable by any of the processes described here below.
In general, the process for the production of the pharmaceutical dosage form according to the invention preferably comprises the following steps:
(a) mixing all ingredients;
(b) optionally pre-forming the mixture obtained from step (a), preferably by applying heat and/or force to the mixture obtained from step (a), the quantity of heat supplied preferably not being sufficient to heat the polyalkylene oxide (C) up to its softening point;
(c) hardening the mixture by applying heat and force, it being possible to supply the heat during and/or before the application of force and the quantity of heat supplied being sufficient to heat the polyalkylene oxide (C) at least up to its softening point;
(d) optionally singulating the hardened mixture;
(e) optionally shaping the pharmaceutical dosage form; and (f) optionally providing a film coating.
Heat may be supplied directly, e.g. by contact or by means of hot gas such as hot air, or with the assistance of ultrasound. Force may be applied and/or the pharmaceutical dosage form may be shaped for example by direct tabletting or with the assistance of a suitable extruder, particularly by means of a screw extruder equipped with two screws (twin-screw-extruder) or by means of a planetary gear extruder.
The final shape of the pharmaceutical dosage form may either be provided during the hardening of the mixture by applying heat and force (step (c)) or in a subsequent step (step (e)). In both cases, the mixture of all components is preferably in the plastified state, i.e.
preferably, shaping is performed at a temperature at least above the softening point of the polyalkylene oxide (C). However, extrusion at lower temperatures, e.g. ambient temperature, is also possible and may be preferred.
Shaping can be performed, e.g., by means of a tabletting press comprising die and punches of appropriate shape.
A particularly preferred process for the manufacture of the pharmaceutical dosage form of the invention involves hot-melt extrusion. In this process, the pharmaceutical dosage form according to the invention is produced by thermoforming with the assistance of an extruder, preferably without there being any observable consequent discoloration of the extrudate. It has been surprisingly found that acid (B) is capable of suppressing discoloration. In the absence of acid (B), the extrudate tends to develop beige to yellowish coloring whereas in the presence of acid (B) the extrudates are substantially colorless, i.e.
white.
This process is characterized in that a) all components are mixed, b) the resultant mixture is heated in the extruder at least up to the softening point of the polyalkylene oxide (C) and extruded through the outlet orifice of the extruder by application of force, c) the still plastic extrudate is singulated and formed into the pharmaceutical dosage form or d) the cooled and optionally reheated singulated extrudate is formed into the pharma-ceutical dosage form.
Mixing of the components according to process step a) may also proceed in the extruder.
The components may also be mixed in a mixer known to the person skilled in the art. The mixer may, for example, be a roll mixer, shaking mixer, shear mixer or compulsory mixer.
Before blending with the remaining components, polyalkylene oxide (C) is preferably provided according to the invention with an antioxidant, preferably a-tocopherol. This may proceed by mixing the two components, the polyalkylene oxide (C) and the antioxidant, preferably by dissolving or suspending the antioxidant in a highly volatile solvent and homogeneously mixing this solution or suspension with polyalkylene oxide (C) and removing the solvent by drying, preferably under an inert gas atmosphere.
The, preferably molten, mixture which has been heated in the extruder at least up to the softening point of polyalkylene oxide (C) is extruded from the extruder through a die with at least one bore.
The process according to the invention requires the use of suitable extruders, preferably screw extruders. Screw extruders which are equipped with two screws (twin-screw-extruders) are particularly preferred.
The extrusion is preferably performed so that the expansion of the strand due to extrusion is not more than 30%, i.e. that when using a die with a bore having a diameter of e.g. 6 mm, the extruded strand should have a diameter of not more than 8 mm. More preferably, the expansion of the strand is not more than 25%, still more preferably not more than 20%, most preferably not more than 15% and in particular not more than 10%.
Preferably, extrusion is performed in the absence of water, i.e., no water is added. However, traces of water (e.g., caused by atmospheric humidity) may be present.
The extruder preferably comprises at least two temperature zones, with heating of the mixture at least up to the softening point of the polyalkylene oxide (C) proceeding in the first zone, which is downstream from a feed zone and optionally mixing zone. The throughput of the mixture is preferably from 1.0 kg to 15 kg/hour. In a preferred embodiment, the throughput is from 1 to 3.5 kg/hour. In another preferred embodiment, the throughput is from 4 to 15 kg/hour.
In a preferred embodiment, the die head pressure is within the range of from 25 to 100 bar.
The die head pressure can be adjusted inter alia by die geometry, temperature profile and extrusion speed.
The die geometry or the geometry of the bores is freely selectable. The die or the bores may accordingly exhibit--a round, oblong or-oval cross-section, wherein-the round cross-section preferably has a diameter of 0.1 mm to 15 mm and the oblong cross-section preferably has a maximum lengthwise extension of 21 mm and a crosswise extension of 10 mm.
Preferably, the die or the bores have a round cross-section. The casing of the extruder used according to the invention may be heated or cooled. The corresponding temperature control, i.e.
heating or cooling, is so arranged that the mixture to be extruded exhibits at least an average temperature (product temperature) corresponding to the softening temperature of the polyalkylene oxide (C) and does not rise above a temperature at which the opioid (A) to be processed may be damaged. Preferably, the temperature of the mixture to be extruded is adjusted to below 180 C, preferably below 150 C, but at least to the softening temperature of polyalkylene oxide (C). Typical extrusion temperatures are 120 C and 130 C.
In a preferred embodiment, the extruder torque is within the range of from 30 to 95%.
Extruder torque can be adjusted inter alia by die geometry, temperature profile and extrusion speed.
After extrusion of the molten mixture and optional cooling of the extruded strand or extruded strands, the extrudates are preferably singulated. This singulation may preferably be performed by cutting up the extrudates by means of revolving or rotating knives, water jet cutters, wires, blades or with the assistance of laser cutters.
Preferably, intermediate or final storage of the optionally singulated extrudate or the final shape of the pharmaceutical dosage form according to the invention is performed under oxygen-free atmosphere which may be achieved, e.g., by means of oxygen-scavengers.
The singulated extrudate may be press-formed into tablets in order to impart the final shape to the pharmaceutical dosage form.
The application of force in the extruder onto the at least plasticized mixture is adjusted by controlling the rotational speed of the conveying device in the extruder and the geometry thereof and by dimensioning the outlet orifice in such a manner that the pressure necessary for extruding the plasticized mixture is built up in the extruder, preferably immediately prior to extrusion. The extrusion parameters which, for each particular composition, are necessary to give rise to a pharmaceutical dosage form with desired mechanical properties, may be established by simple preliminary testing.
For example but not limiting, extrusion may be performed by means of a twin-screw-extruder type ZSE 18 or ZSE27 (teistritz, Nurnberg, Germany), screw diameters of 18 or 27- mm.
Screws having eccentric ends may be used. A heatable die with a round bore having a diameter of 7, 8, or 9 mm may be used. The extrusion parameters may be adjusted e.g. to the following values: rotational speed of the screws: 120 Upm; delivery rate2 kg/h for a ZSE
18 or 8 kg/h for a ZSE27; product temperature: in front of die 125 C and behind die 135 C;
and jacket temperature: 110 C.
Preferably, extrusion is performed by means of twin-screw-extruders or planetary-gear-extruders, twin-screw extruders (co-rotating or contra-rotating) being particularly preferred.
The pharmaceutical dosage form according to the invention is preferably produced by thermoforming with the assistance of an extruder without any observable consequent discoloration of the extrudates.
The process for the preparation of the pharmaceutical dosage form according to the invention is preferably performed continuously. Preferably, the process involves the extrusion of a homogeneous mixture of all components. It is particularly advantageous if the thus obtained intermediate, e.g. the strand obtained by extrusion, exhibits uniform properties.
Particularly desirable are uniform density, uniform distribution of the active compound, uniform mechanical properties, uniform porosity, uniform appearance of the surface, etc.
Only under these circumstances the uniformity of the pharmacological properties, such as the stability of the release profile, may be ensured and the amount of rejects can be kept low.
A further aspect of the invention relates to a packaging containing a pharmaceutical dosage form according to the invention and an oxygen scavenger. Suitable packages include blister packages and bottles, such as glass bottles or bottles made from thermoplastic polymers.
Suitable oxygen scavengers are known to the skilled artisan. The oxygen scavenger can be any scavenger known in the art to scavenge oxygen. Both organic and inorganic oxygen scavengers can be used.
In one embodiment, the oxygen scavenger is any metal complex exhibiting oxygen scavenging activity. Examples include complexes containing one or more of aluminum, aluminum ferrosilicon, antimony, beryllium, calcium silicon, cerium, cobalt, gallium, hafnium, iron, magnesium alloy, nickel catalyst, selenium, silicon, silver, strontium, titanium, zinc, and/or zirconium.
In yet another embodiment, one or more elements from Group IA of the periodic table and their alloys and compounds may be used as oxygen scavengers. Examples of Group IA
elements include cesium, lithium, potassium, sodium. Further examples of inorganic oxygen scavengers include one or more of sodium azide (NaN3), sodium sulfite (Na2SO3), hydrazine, and hydroxylamine.
In one embodiment, the oxygen scavenger is an organic compound. Examples include one or more of the polyterpenes, ascorbic acid, amino polycarboxylic acid, cyclohexanedione, tetramethyl piperidone, and heterocyclic compounds with N-substituted amino groups.
Oxygen scavengers and the application thereof in pharmaceutical packaging are known to the skilled artisan. In a preferred embodiment, the oxygen scavenger is selected from the group consisting of metal-catalyzed oxidizable organic polymers and anti-oxidants. Particularly preferred are those oxygen scavengers that are able to perform in a dry environment of below 60% relative humidity, preferably below 30%
relative humidity and that are combined with a dessicant. Examples of commercially available oxygen scavengers satisfying these requirements include Pharmakeep KD10 and KD20.
It has been surprisingly found that the storage stability of the pharmaceutical dosage form can be increased when keeping the oxygen content of the atmosphere within the packaging low. Methods for packaging pharmaceutical dosage forms and the application of suitable oxygen scavengers are known to the skilled artisan. In this regard it can be referred to e.g.
D.A. Dean, Pharmaceutical Packaging Technology, Taylor & Francis, 1st ed.;
F.A. Paine et al., Packaging Pharmaceutical and Healthcare Products, Springer, 1st ed.; and O.G. Piringer et al., Plastic Packaging: Interactions with Food and Pharmaceuticals, Wiley-VCH, 2nd ed.
As far as the packaging is concerned, round bottles made from polyolefins, preferably from HDPE, are preferred. The thickness of the bottle wall is preferably at least 0.25 mm, more preferably at least 0,5 mm, otherwise the bottle may collapse.
As far as the lid of the packaging is concerned, the packaging is preferably induction or heat-sealed with an aluminium foil.
It has been surprisingly found that by selecting an appropriate shape of the packaging and sealing, the vacuum that is produced by the effect of the oxygen scavenger (underpressure of about 20,000 Pa = 2 N/cm2) can be handled without causing a collapse of the packaging.
Induction sealing (e.g. 3 seconds energy) is preferred. When sealing a 75 ml bottle having an opening with a diameter of 1 inch with aluminium foil, an underpressure of 20,000 Pa due to oxygen scavenging results in a force of about 10 N corresponding to the force that is exerted by a weight of 1 kg.
The mechanical stability of the sealing can be tested either by introducing an appropriate amount of oxygen scavenger in the bottle, sealing it and waiting for a sufficient period of time, e.g. 2 days, so that the oxygen is scavenged and an underpressure of about 20,000 Pa has been developed. Alternatively, the bottle may be sealed without any oxygen scavenger in its interior and a weight of 1 kg can be placed on the aluminium foil externally thus, simulating the force.
A further aspect of the invention relates to the use of an opioid (A) for the manufacture of the pharmaceutical dosage form as described above for the treatment of pain.
A further aspect of the invention relates to the use of a pharmaceutical dosage form as described above for avoiding or hindering the abuse of the opioid (A) contained therein.
A further aspect of the invention relates to the use of a pharmaceutical dosage form as described above for avoiding or hindering the unintentional overdose of the opioid (A) contained therein.
In this regard, the invention also relates to the use of a opioid (A) as described above and/or a polyalkylene oxide (C) as described above for the manufacture of the pharmaceutical dosage form according to the invention for the prophylaxis and/or the treatment of a disorder, thereby preventing an overdose of the opioid (A), particularly due to comminution of the pharmaceutical dosage form by mechanical action.
Further, the invention relates to a method for the prophylaxis and/or the treatment of a disorder comprising the administration of the pharmaceutical dosage form according to the invention, thereby preventing an overdose of the opioid (A), particularly due to comminution of the pharmaceutical dosage form by mechanical action. Preferably, the mechanical action is selected from the group consisting of chewing, grinding in a mortar, pounding, and using apparatuses for pulverizing conventional pharmaceutical dosage forms.
The following examples further illustrate the invention but are not to be construed as limiting its scope.
Example 1 Tablets were prepared by hot-melt extrusion of various homogeneous constituent mixtures under the following, identical extrusion conditions:
extruder type: Leistritz Extruder ZSE18PH 40D equipped with high shear screws and a die of 9 mm diameter throughput: 1.0 kg/h revolution velocity: 100 rpm barrel temperature: 100 C
extrudate temperature: 120 C
The extrudate was cut into slices of 325 mg containing about 5 mg oxymorphone hydrochloride.
The individual constituents of the extruded mixtures as well as the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.-%) decomposition products ex. further ingredient (wt.-%) wt.-%
(A) PEO PEG HPMC a-toc. oNo' oNo2 E' E2 Al 1.5 76.9 10.0 10.0 1.5 I 0.06 0.58 0.41 1.93 A2 1.5 77.5 10.0 10.0 1.0 I 0.09 0.49 0.58 1.81 A3 1.5 78.0 10.0 10.0 0.5 / 0.08 0.36 0.56 1.64 A4 1.5 78.3 10.0 10.0 0.2 I 0.08 0.26 0.63 1.51 A5 1.5 78.5 10.0 10.0 0.0 I 0.07 0.17 0.81 1.69 Bi 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 B2 1.5 .40.0 10.0 46.9 1.5 / 0.09 0.55 0.64 1.76 B3 1.5 50.0 10.0 36.9 1.5 / 0.00 0.52 0.29 1.64 B4 1.5 50.0 36.9 10.0 1.5 / 0.11 0.76 0.36 1.74 C1 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 C2 1.5 76.9 / 10.0 1.5 10.00 Lutrol F68 0.05 0.53 0.65 1.83 C3 1.5 50.0 10.0 10.0 1.5 26.90 mannitol 0.08 0.82 0.39 2.72 C4 1.5 76.9 / 10.0 1.5 10.00 carnaubawax 0.12 0.53 0.39 1.03 Di 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 D2 1.5 76.8 10.0 10.0 1.5 0.10 fumaric acid 0.05 0.48 0.52 1.70 D3 1.5 76.8 10.0 10.0 1.5 0.10 Na-EDTA 0.07 0.51 0.48 1.77 D4 1.5 76.8 10.0 10.0 1.5 0.10 citric acid 0.07 0.48 0.37 1.45 El 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 E2 1.5 76.8 10.0 10.0 1.5 0.10 citric acid 0.07 0.48 0.37 1.45 E3 1.5 76.7 10.0 10.0 1.5 0.20 citric acid 0.00 0.40 0.20 1.13 Ea - 1.5-176.4 10.0- 10:0 --- -1:5 -- _0:50 citric acid-- - -0.00 - 0.06--0:12 _ 0:17--_ _ (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities ' after extrusion, before storage 2.
after storage, amber glass bottles, plastic cap, 4 weeks, 40 C, 75% rel.
humidity The decomposition products were analyzed by HPLC-UV. The elution peak for oxymor-phone-N-oxide could not be sufficiently base-line separated from a peak of an unknown degradation product (called "UK 0.83"). Thus, both peaks were jointly integrated. It becomes evident from a comparison of examples A, to A5 that the content of oxymorphone-N-oxide before storage (oNo') is not substantially changed when the content of antioxidant a-tocopherol is decreased from 1.5 wt.-% to 1.0 wt.-%, 0.5 wt.-%, 0.2 wt.-% and even 0 wt.-%.
Upon storage (oNo2), however, the content of oxymorphone-N-oxide is proportional to the content of a-tocopherol. This is most surprising because oxymorphone-N-oxide is an oxidation product and one would expect that antioxidants usually rather suppress than support the formation of oxidation products.
Nonetheless, the complete omission of antioxidant ((x-tocopherol) has disadvantages. It could be shown by viscosity measurements that the high molecular polyethylene oxide is degraded upon extrusion and/or storage in the absence of antioxidant. It has been surpri-singly found that about 0.2 wt.-% a-tocopherol suffice in order to stabilize the polyethylene oxide; higher contents of a-tocopherol do not result in higher viscosities of the polyalkylene oxide and, thus, do not prevent PEO more pronounced from degradation. Thus, the content of antioxidant (a-tocopherol) is preferably balanced so that on the one side, the high molecular weight polyethylene oxide is sufficiently stabilized and that on the other side, the undesired formation of oxymorphone-N-oxide is kept low during storage.
Further, it becomes evident from a comparison of examples B, to B4 and examples C, to C4 that the partial replacement of the high molecular weight polyethylene oxide or the total replacement of the polyethylene glycol by an alternative plasticizer does not result in a substantial decrease of the content of undesired oxymorphone-N-oxide. This is surprising because one would expect that polyethylene oxide and polyethylene glycol are potential peroxide carriers and that a reduction thereof would result in a reduction of oxidative processes such as the oxidation of oxymorphone to oxymorphone-N-oxide.
Still further, it becomes evident from a comparison of examples D, to D5 and E, to E4 that the addition of physiologically acceptable acids, particularly citric acid, leads to a reduction of the formation of oxymorphone-N-oxide. This effect is more pronounced when the amount of acid is increased. At a concentration of 0.1 wt.-%, the effect is comparatively weak, but at a con-centration of 0.2 wt.-% the effect is stronger and is further enhanced when the concentration of citric acid is increased. Not only the amount of oxymorphone-N-oxide is decreased, but also the total amount of decomposition products, particularly of those having high HPLC
retention times.
Example 2 Tablets that had been manufactured in analogy to ex. A,, B,, C1, D, and E, above were packaged in different packaging materials and stored at 40 C and 75% rel.
humidity. The decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
w0 0 0 0 0 0 0 0 L Y M O co o 0 0 -, o CO "t E 17 M O M M co E cn 0 M 0) Co C o 0 0 0 m y y + Yco 0 0 C
0 r-- m Coo rC i O o co U) v ~n C) M It 00 ce) o 0 0 0 Y rn \ o 0 a) CC) 0 ~t 0) a N E 0 0) N N I- 0 N- 0) co co 0) 0 CO O O O
(6 L U
E ui fu 'a) Y 0 0 0` \ \0 \ \ \
0) a) C`! 0 0) CO
0N E 0 in Cn M M M Ch Cl) V M 0) 0) 0 O O O O
C
co + Y Lo 0 0 Q
CO C a) C-4 CO cq Co It co N co 0 CM C4 co M O O O O O
N
(D cu E L) C N
a) (n -0 0) Y M o 0 N cli M Co 0) CO N
O XO Cn E O O Lo c) O O co p M 0) 00) 0 O O O O O o 04 N (n U) O O O 2 O O O 2 a Q) N O o v o 0 0 0 0 N U) UC 0 co LO M to p) co E u-) r 0 r u -le CO co CO 0) W O N N N
L
E co co Y 0 CD 0 0 0 0 0 o a C O O co N Cl) M E M lf) f COO Cl) o v Cc\l )) rn co 0) 0 0 0 O. 3 a) 0) Y E o 0o 0 0 0 o a) -O y LQ C~l "I: cq 0 CO O 0 CO 4 M .
CD = N 0 N CO N co 0) 00) O .- O M N
to E M C
v LLj =2 0) E 0) x0 E o 0 0 co 0 o 0 O 't O co qq- N
CO O CD co N
O N 0) 0) ) O O O O N ~
M E
.". LC) C, Co I-O C`u M M CO CO 0) O 0) M 0 M 00) 0) O O O O O E
O
c Cl) O 0 6 M W N
0 O X c O N
-c L O
Q- L O L
O CL O Z M o 0 E o 0 CO
0 (n x >, co o E - E
0 t5 0 L Y >, X cu c y- 0 o o a) 'co o O.- E E w C) o o t It has been surprisingly found that inclusion of an oxygen scavenger in the packaging results in a further stabilization of the dosage form so that the formation of decomposition products is limited to extremely low values.
Example 3:
Tablets were manufactured as described in example 1, packed into HDPE bottles of 75 ml volume together with an oxygen scavenger combined with a desiccant (Pharmakeep 20 KD), closed with a plastic cap with induction seal.
The individual constituents of the extruded mixtures, the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.-%) decomposition products ex. (wt.-%) (A) PEO PEG HPMC a-toc. Citric acid oNo' oNo2 oNo3 E' E2 E' F, 1.5 73.8 10.0 14.0 0.2 0.5 nd nd nd nd nd 0.05 F2 1.5 77.8 10.0 10.0 0.2 0.5 nd nd Ind nd 0.05 0.10 (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities after extrusion, before storage 2: after storage, HDPE bottles, plastic cap with induction seal, oxygen scavenger, 4 weeks, 40 C, 75% rel. humidity 3 after storage, HDPE bottles, plastic cap with induction seal, oxygen scavenger, 8 weeks, 40 C, 75% rel. humidity The results reveal that the purity of the product is very high after manufacturing and that the product exhibit stable during 8 weeks storage under accelerated conditions of 40 C/75% rel.
humidity.
Example 4:
Tablets were manufactured as described in example 1 but cut into slices of 215 mg representing 5 mg or 40 mg of oxymorphone HCl, after forming the tablets were coated with about 6.5 mg each of a conventional Opadry II film-coat containing polyvinylalcohol as the film forming excipient, packed into HDPE bottles of 75 ml volume together with an oxygen scavenger combined with a desiccant (Pharmakeep 20 KD), closed with a plastic cap with induction seal.
The individual constituents of the extruded mixtures, the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.-%) decomposition products ex. (wt.-%) ffG,2~33 PEO PEG HPMC a-toc. Citric acid oNo' oNo2 E' E2 70.0 16.63 10.0 0.2 0.84 nd nd nd nd 56.8 13.56 10.0 0.2 0.84 nd nd 0.05 0.05 (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC : hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities ' = after extrusion, before storage 2: after storage, HDPE bottles, plastic cap with induction seal, oxygen scavenger, 1 month, 40 C, 75% rel. humidity Example 5:
The most preferred dosage form according to example 3 is also suitable for the stabilization of oxycodone. This could be demonstrated for a formulation containing 80 mg of oxycodone HCI manufactured analogue to example 1 but, the extrudate was cut into slices of 400 mg:
constituents (wt.-%) decomposition products ex. wt.-%
(A) PEO PEG HPMC a-toc. Citric acid oNo' oNo2 Z2 H, 20 54.3 15 10 0.2 0.5 0.06 0.07 0.22 0.13 (A): oxycodone PEO : polyethylene oxide MH, 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxycodone-N-oxide (Impurity D+E) ' : after extrusion, before storage 2: after storage, amber glass bottles, plastic cap, oxygen scavenger with desiccant (Pharmakeep 20KD) 1 month, 40 C, 75% rel. humidity Example 6:
In a single dose (40 mg oxymorphone HCI, tablets of example 4), randomized, three-way crossover study with 1 week between treatments subjects were fasted overnight and meals were served 4 and 10 hours after dosing. No water was given within 1 hour of dosing. All tablets were taken with 240 mL of water (example T).
PK samples were taken for oxymorphone and 6-OH-oxymorphone predose and up through 48 hours after dosing.
Bioequivalence was compared to Opana ER (reference R).
The results are summarized in the tables here below:
Treatment Mean SD CV
Cm,, [pg/m L] T 2147 989 46%
R 2671 1163 44%
AUCT [pg*h/m L] T 38695 13836 36%
R 38171 14652 38%
AUC [pg*h/m L] T 42575 15836 37%
R 41296 15242 37%
Point Estimate T/R Lower Limit 90% Cl Upper Limit 90% Cl Cmax 79.37 71.69 87.87 AUCT 101.98 95.17 109.29 AUC 102.24 95.48 109.48 Cl = confidence interval It becomes evident that the dosage forms according to the invention having an increased breaking strength are bioequivalent to conventional dosage forms (Opana ER ).
Example 7 Tablets were prepared under identical conditions by hot-melt extrusion of two homogeneous constituent mixtures I, and 12:
I, 12 O mor hone HCI [%] 11.1 11.1 PEO [%] 68.2 63.2 PEG [%] 10.0 15.0 HPMC Shin Etsu [%] 10.0 10.0 a-toco hero) [%] 0.2 0.2 Citric acid, anhydrous [%] 0.5 0.5 Tablet weight [mg] 360 360 PEO:PEG 6.82: 1 4.21 : 1 under the following, identical extrusion conditions:
extruder type: Leistritz Extruder type Micro 27 GL 40 D equipped with medium shear screws and a die of 8 mm diameter throughput: 10 kg/h revolution velocity: 120 rpm manufacturing time: 30 min temperature of hottest heating zone: 100 C
die temperature: 130 C.
The extrudate was cut into slices of 360 mg containing about 40 mg oxymorphone hydrochloride.
100 slices were weighed individually and the standard deviation of weight was calculated.
Slices of composition I, (PEO:PEG = 6.82:1) showed a standard deviation of 2.3 %, whereas slices of composition 12 (PEO:PEG = 4.21:1) showed a standard deviation of 1.6 % only.
It becomes evident from these comparative tests that surprisingly, the processability of the extruded mass can be improved by adjusting the ratio of PEO to PEG.
Example 8 In order to investigate if also multicarboxylic acids other than citric acid could hamper the formation of oxymorphone-N-oxide, tablets containing maleinic acid or fumaric acid were manufactured as described in example 1. For comparison, also tablets containing the inorganic salt NaH2PO4 were manufactured. The samples were stored in open dishes at 40 C and 75% relative humidity for 4 weeks.
The individual constituents of the extruded mixtures as well as the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.%) decomposition products wt.%
ex. further ingredient (wt.-%) (A) PEO PEG HPMC a-toc. oNo' oNo2 E' Y2 J, 1.5 76.0 10.0 10.0 1.5 Maleinic acid 1.0 % Ind nd 0.20 0.22 J2 1.5 76.0 10.0 10.0 1.5 Fumaric acid 1.0 % nd nd 0.17 0.30 J3 1.5 76.0 10.0 10.0 1.5 NaH2PO41.0 %* nd 0.18 0.06 0.75 (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol *NaH2PO4: Used in form of 1.3% of the di-hydrate oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities; maleinic acid, fumaric acid and related compounds subtracted from sum of impurities after extrusion, before storage 2: after storage, open dish, 4 weeks, 40 C, 75% rel. humidity In case of maleinic and fumaric acid these compounds and for maleinic acid another related compound were detected during the purity tests as impurities (up to about 40%). Their values have been subtracted from the sum of impurities It becomes evident from a comparison of examples J, and J2 to A, and B, that the presence of maleinic and fumaric acid protected oxymorphone totally against oxidation to N-oxide and to a large extent against other degradation although the samples were stored in open dishes and not in closed bottles. These results are comparable to those obtained with citric acid (example 1, D4 and E2-E4). Samples containing NaH2PO4 (J3) exhibited protection against N-oxide formation and other degradation when compared to the formulations without any acidic compound (A, and B,) but to a less extent than the multicarboxylic acids like citric, maleinic and fumaric acid.
Example 9 In order to investigate if the presence of citric acid also protects oxidation sensitive opioids other than oxymorphone against N-oxidation, tablets containing oxycodone hydrochloride were manufactured as described in example 1.
For comparison, also tablets containing smaller amounts of a-tocopherol were manufactured.
The samples were stored in open dishes at 40 C and 75% relative humidity for 4 weeks.
The individual constituents of the extruded mixtures as well as the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.%) decomposition products ex. further ingredient (wt.%) wt.%
(A) PEO PEG HPMC a-toc. oNo' oNo2 E' E2 K, 1.5 77.0 10.0 10.0 1.5 / 0.05 0.58 0.31 1.63 K2 1.5 78.3 10.0 10.0 0.2 / 0.05 0.28 0.58 0.69 K3 1.5 76.0 10.0 10.0 1.5 Citric acid 1.0 nd nd 0.19 0.22 K4 1.5 77.3 1Ø0 1Ø0 _0.2 - Citricacid 1.0 nd- - - nd 0.18 0.23 (A) : oxycodone hydrochloride PEO : polyethylene oxide M,, 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxycodone-N-oxide E: sum of all impurities after extrusion, before storage 2 : after storage, open dish, 4 weeks, 40 C, 75% rel. humidity These results show that citric acid protected oxycodone totally against oxidation to the N-oxide and to a large extent against other degradation although the samples were stored in open dishes rather than in closed bottles. Reducing the amount of a-tocopherol resulted in reduced degradation, when formulations were employed not containing citric acid. These results are comparable to those obtained with oxymorphone.
In another preferred embodiment, the further polymer is a cellulose ester or cellulose ether, preferably HPMC, having a content within the range of 14 8 wt.-%, more preferably 14 6 wt.-%, still more preferably 14 5 wt.-%, yet more preferably 14 4 wt.-%, most preferably 14 3 wt.-%, and in particular 14 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
All polymers are preferably employed as powders. They can be soluble in water.
Besides the opioid (A), the acid (B) and polyalkylene oxide (C) the pharmaceutical dosage form according to the invention may contain further constituents, such as conventional pharmaceutical excipients.
Preferably, the pharmaceutical dosage form comprises an antioxidant. Suitable antioxidants include ascorbic acid, a-tocopherol (vitamin E), butylhydroxyanisol, butylhydroxytoluene, salts of ascorbic acid (vitamin C), ascorbylic palmitate, monothioglycerine, coniferyl benzoate, nordihydroguajaretic acid, gallus acid esters, phosphoric acid, and the derivatives thereof, such as vitamin E-succinate or vitamin E-palmitate and/or sodium bisulphite, more preferably butyihydroxytoluene (BHT) or butylhydroxyanisol (BHA) and/or a-tocopherol.
Preferably, the content of the antioxidant is within the range of from 0.001 to 5.0 wt.-%, more preferably 0.002 to 2.5 wt.-%, more preferably 0.003 to 1.5 wt.-%, still more preferably 0.005 to 1.0 wt.-%, yet more preferably 0.01 to 0.5 wt.-%, most preferably 0.05 to 0.4 wt.-% and in particular 0.1 to 0.3 wt.-%, based on the total weight of the pharmaceutical dosage form.
A particularly preferred antioxidant is a-tocopherol. It has been surprisingly found that a-tocopherol stabilizes polyalkylene oxide and simultaneously destabilizes certain opioids (A), such as oxymorphone. Thus, in a preferred embodiment, the content of a-tocopherol is balanced between a sufficient stability of the polyalkylene oxide on the one hand and a sufficient stability of the opioid (A) on the other hand.
In a preferred embodiment, the content of a-tocopherol is within the range of 0.2 0.18 wt.-%, more preferably 0.2 0.15 wt.-%, still more preferably 0.2 0.12 wt.-%, yet more preferably 0.2 0.09 wt.-%, most preferably 0.2 0.06 wt.-%, and in particular 0.2 0.03 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the relative weight ratio of the acid (B), preferably citric acid, and the antioxidant, preferably a-tocopherol, is within the range of from 10:1 to 1:10, more preferably 8:1 to 1:8, still more preferably 6:1 to 1:6, yet more preferably 5:1 to 1:4, most preferably 4:1 to 1:3 and in particular 3:1 to 1:2.
The pharmaceutical dosage form according to the invention may also contain a natural, semi-synthetic or synthetic wax. Waxes with a softening point of at least 50 C, more preferably 60 C are preferred. Carnauba wax and beeswax are particularly preferred, especially carnauba wax.
Preferably, the release profile of the opioid (A) is matrix-retarded.
Preferably, the opioid (A) is embedded in a matrix comprising the polyalkylene oxide, said matrix controlling the release of the opioid (A) from the pharmaceutical dosage form.
Physiologically acceptable materials which are known to the person skilled in the art may be used as supplementary matrix materials. Polymers, particularly preferably cellulose ethers, cellulose esters and/or acrylic resins are preferably used as hydrophilic matrix materials.
Ethylcellulose, hydroxypropylmethylcellulose, hyd roxypro pylcel I u lose, hydroxymethylcellu-lose, hydroxyethylcellulose, poly(meth)acrylic acid and/or the derivatives thereof, such as the salts, amides or esters thereof are very particularly preferably used as matrix materials.
Matrix materials prepared from hydrophobic materials, such as hydrophobic polymers, waxes, fats, long-chain fatty acids, fatty alcohols or corresponding esters or ethers or mixtures thereof are also preferred. Mono- or diglycerides of C12-C30 fatty acids and/or C12-C30 fatty alcohols and/or waxes or mixtures thereof are particularly preferably used as hydrophobic materials. It is also possible to use mixtures of the above-stated hydrophilic and hydrophobic materials as matrix materials.
Preferably, the relative weight ratio of the polyalkylene oxide to the opioid (A) is at least 0.5:1, more preferably at least 1:1, at least 2:1, at least 3:1, at least 4:1, at least 5:1, at least 6:1, at least 7:1, at least 8:1 or at least 9:1; still more preferably at least 10:1 or at least 15:1, yet more preferably at least 20:1, most preferably at least 30:1 and in particular at least 40:1.
In a preferred embodiment, the relative weight ratio of the polyalkylene oxide to the opioid (A) is within the range of from 3:1 to 50:1, more preferably 3:1 to 40:1 and in particular 3:1 to 30:1.
The pharmaceutical dosage form according to the invention preferably contains a plasticizer.
The plasticizer improves the processability of the polyalkylene oxide. A
preferred plasticizer is polyalkylene glycol, like polyethylene glycol, triacetin, fatty acids, fatty acid esters, waxes and/or microcrystalline waxes. Particularly preferred plasticizers are polyethylene glycols, such as PEG 6000.
Preferably, the content of the plasticizer is within the range of from 0.1 to 25 wt.-%, more preferably 0.5 to 22.5 wt.-%, still more preferably 1.0 to 20 wt.-%, yet more preferably 2.5 to 17.5 wt.-%, most preferably 5.0 to 15 wt.-% and in particular 7.5 to 12.5 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the plasticizer is a polyalkylene glycol having a content within the range of 10 8 wt.-%, more preferably 10 6 wt.-%, still more preferably 10 5 wt.-%, yet more preferably 10 4 wt.-%, most preferably 10 3 wt.-%, and in particular 10 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
In another preferred embodiment, the plasticizer is a polyalkylene glycol having a content within the range of 15 8 wt.-%, more preferably 15 6 wt.-%, still more preferably 15 5 wt.-%, yet more preferably 15 4 wt.-%, most preferably 15 3 wt.-%, and in particular 15 2 wt.-%, based on the total weight of the pharmaceutical dosage form.
In a preferred embodiment, the relative weight ratio of the polyalkylene oxide to the polyalkylene glycol is within the range of 4.2 2 : 1, more preferably 4.2 1.5 : 1, still more preferably 4.2 1 : 1, yet more preferably 4.2 0.5 : 1, most preferably 4.2 0.2 : 1, and in particular 4.2 0.1 : 1. This ratio satisfies the requirements of relative high polyalkylene oxide content and good extrudability.
When manufacturing the dosage forms from slices that are obtained by cutting the extrudate strand, the weight of the slices determines the weight of the resulting dosage form.
Pronounced variation in weight of these slices results in an accordant weight deviation of dosage forms from the target weight. The weight variation of slices depends strongly on the surface properties of the extrudate strand. A strand with a thoroughly smooth surface allows the generation of slices exhibiting a low weight variation. In contrast, a wavy or shark skinning strand results in slices exhibiting a higher weight variation thereby increasing the number of rejects.
It has now been surprisingly found that the surface properties of the extrudate strand can be triggered by the polyalkylene oxide : polyalkylene glycol weight ratio.
Preferred compositions X, to X32 of the pharmaceutical dosage form according to the invention are summarized in the tables here below:
wt.% X, X2 X3 X4 o ioid (A) (e.g. ox mo hone HCI) 1.50 1.25 1.50 1.00 1.50 0.75 1.50 0.50 acid (B) (e.g. citric acid) 0.5 0.30 0.5 0.25 0.5 0.20 0.5 0.15 of alk lene oxide (C) 77 22 77 20 77 15 77 10 cellulose ester or ether (e.g. HPMC) 12 10 12 7.5 12 5 12 2.5 -plasticizer (e.g. PEG) 10 7.5 10 5 10 2.5 10 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.% X5 X6 X7 X8 o ioid (A) (e.g. ox mo hone HCI) 2.33 1.25 2.33 1.00 2.33 0.75 2.33 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 of alk lene oxide (C) 70 25 70 20 70 15 70 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 -plasticizer (e.g. PEG) 16.6 7.5 16.6 5 16.6 2.5 16.6 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.% X9 X10 X11 X12 opioid (A) (e.g. ox mo hone HCI) 3.50 1.25 3.50 1.00 3.50 0.75 3.50 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 of alk lene oxide (C) 69 30 69 20 69 15 69 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 16.4 7.5 16.4 5 16.4 2.5 16.4 1.0 antioxidant (e.g. a-toco herol 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.% X13 X14 X15 X16 opioid (A) (e.g. ox mo hone HCI) 4.65 1.25 4.65 1.00 4.65 0.75 4.65 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 68 30 68 20 68 15 68 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 16.2 7.5 16.2 5 16.2 2.5 16.2 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 opioid (A) (e.g. ox mo hone HCI) 6.98 1.25 6.98 1.00 6.98 0.75 6.98 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 of alk lene oxide (C) 66 30 66 20 66 15 66 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 15.8 7.5 15.8 5 15.8 2.5 15.8 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.-% X21 X22 X23 X24 opioid (A) (e.g. ox mo hone HCI) 9.30 1.25 9.30 1.00 9.30 0.75 9.30 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 64 30 64 20 64 15 64 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 15.3 7.5 15.3 5 15.3 2.5 15.3 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.-% X25 X26 X27 X28 opioid (A) (e.g. ox mo hone HCI 13.95 1.25 13.95 1.00 13.95 0.75 13.95 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 60 30 60 20 60 15 60 10 cellulose ester or ether (e.g. HPMC) 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 13.9 7.5 13.9 5 13.9 2.5 13.9 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 wt.-% X29 X3o X31 X32 opioid (A) (e.g. ox mo hone HCI) 18.60 1.25 18.60 1.00 18.60 0.75 18.60 0.50 acid (B) (e.g. citric acid) 0.85 0.60 0.85 0.50 0.85 0.25 0.85 0.15 polyalkylene oxide (C) 57 30 57 20 57 15 57 10 cellulose ester or ether (e.g. HPMC 10 9.5 10 7.5 10 5 10 2.5 plasticizer (e.g. PEG) 13.6 7.5 13.6 5 13.6 2.5 13.6 1.0 antioxidant (e.g. a-toco hero) 0.2 0.12 0.2 0.1 0.2 0.05 0.2 0.03 In a preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 100 75 mg, more preferably 100 50 mg, most preferably 100 25 mg. In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 200 75 mg, more preferably 200 50 mg, most preferably 200 25 mg. In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 250 75 mg, more preferably 250 50 mg, most preferably 250 25 mg. In still another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 300 75 mg, more preferably 300 50 mg, most preferably 300 25 mg. In yet another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 400 75 mg, more preferably 400 50 mg, most preferably 400 25 mg.
In a preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 500 250 mg, more preferably 500 200 mg, most preferably 500 150 mg.
In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 750 250 mg, more preferably 750 200 mg, most preferably 750 150 mg. In another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 1000 250 mg, more preferably 1000 200 mg, most preferably 1000 150 mg. In still another preferred embodiment, the pharmaceutical dosage form has a total weight within the range of 1250 250 mg, more preferably 1250 200 mg, most preferably 1250 150 mg.
In a preferred embodiment, the pharmaceutical dosage form according to the invention has an overall density within the range of 1.19 0.30 g/cm3, more preferably 1.19 0.25 g/cm3, still more preferably 1.19 0.20 g/cm3, yet more preferably 1.19 0.15 g/cm3, most preferably 1.19 0.10 g/cm3, and in particular 1.19 0.05 g/cm3. Preferably, the overall density of the pharmaceutical dosage form according to the invention is 1.17 0.02 g/cm3, 1.19 0.02 g/cm3 or 1.21 0.02 g/cm3. Methods for measuring the density of a dosage form are known to a person skilled in the art. The overall density of a dosage form can for example be determined by means of the mercury porosimetry method or the helium pycnometer method as described in Ph. Eur.
Preferably, the pharmaceutical dosage form according to the invention is adapted for oral administration. It is also possible, however, to administer the pharmaceutical dosage form via different routes and thus, the pharmaceutical dosage form may alternatively be adapted for buccal, lingual, rectal or vaginal administration. Implants are also possible.
In a preferred embodiment, the pharmaceutical dosage form according to the invention is adapted for administration once daily. In another preferred embodiment, the pharmaceutical dosage form according to the invention is adapted for administration twice daily. In still another preferred embodiment, the pharmaceutical dosage form according to the invention is adapted for administration thrice daily.
For the purpose of the specification, "twice daily" means equal or nearly equal time intervals, i.e., about every 12 hours, or different time intervals, e.g., 8 and 16 hours or 10 and 14 hours, between the individual administrations.
For the purpose of the specification, "thrice daily" means equal or nearly equal time intervals, i.e., about every 8 hours, or different time intervals, e.g., 6, 6 and 12 hours; or 7, 7 and 10 hours, between the individual administrations.
Preferably, the pharmaceutical dosage form according to the invention causes an at least partially delayed or prolonged release of opioid (A).
Controlled or prologned release is understood according to the invention preferably to mean a release profile in which the opioid (A) is released over a relatively long period with reduced intake frequency with the purpose of extended therapeutic action. Preferably, the meaning of the term "prolonged release" is in accordance with the European guideline on the nomen-clature of the release profile of pharmaceutical dosage forms (CHMP). This is achieved in particular with peroral administration. The expression "at least partially delayed or prolonged release" covers according to the invention any pharmaceutical dosage forms which ensure modified release of the opioids (A) contained therein. The pharmaceutical dosage forms preferably comprise coated or uncoated pharmaceutical dosage forms, which are produced with specific auxiliary substances, by particular processes or by a combination of the two possible options in order purposefully to change the release rate or location of release.
In the case of the pharmaceutical dosage forms according to the invention, the release time profile of a controlled release form may be modified e.g. as follows: extended release, repeat action release, prolonged release and sustained release.
For the purpose of the specification "controlled release" preferably means a product in which the release of active compound over time is controlled by the type and composition of the formulation. For the purpose of the specification "extended release"
preferably means a product in which the release of active compound is delayed for a finite lag time, after which release is unhindered. For the purpose of the specification "repeat action release" preferably means a product in which a first portion of active compound is released initially, followed by at least one further portion of active compound being released subsequently.
For the purpose of the specification "prolonged release" preferably means a product in which the rate of release of active compound from the formulation after administration has been reduced over time, in order to maintain therapeutic activity, to reduce toxic effects, or for some other therapeutic purpose. For the purpose of the specification "sustained release"
preferably means a way of formulating a medicine so that it is released into the body steadily, over a long period of time, thus reducing the dosing frequency. For further details, reference may be made, for example, to K.H. Bauer, Lehrbuch der Pharmazeutischen Technologie, 6th edition, WVG Stuttgart, 1999; and Eur. Ph.
The pharmaceutical dosage form according to the invention may comprise one or more opioids (A) at least in part in a further controlled release form, wherein controlled release may be achieved with the assistance of conventional materials and processes known to the person skilled in the art, for example by embedding the substance in a controlled release matrix or by applying one or more controlled release coatings. Substance release must, however, be controlled such that addition of delayed-release materials does not impair the necessary breaking strength. Controlled release from the pharmaceutical dosage form according to the invention is preferably achieved by embedding the substance in a matrix.
Preferably, polyalkylene oxide (C) serves as such a matrix. The auxiliary substances acting as matrix materials control release. Matrix materials may, for example, be hydrophilic, gel-forming materials, from which release proceeds mainly by diffusion, or hydrophobic materials, from which release proceeds mainly by diffusion from the pores in the matrix.
Preferably, the release profile is substantially matrix controlled, preferably by embedding opioid (A) in a matrix comprising polyalkylene oxide (C) and optionally, further matrix materials. Preferably, the release profile is not osmotically driven.
Preferably, release kinetics is not zero order.
Preferably, under physiological conditions the pharmaceutical dosage form according to the invention has released after 30 minutes 0.1 to 75%, after 240 minutes 0.5 to 95%, after 480 minutes 1.0 to 100% and after 720 minutes 2:5 to 100% of the opioid (A).
Further preferred release profiles R, to R6 are summarized in the table here below [all data in wt.-% of released opioid (A)]:
time R, R2 R3 R4 R5 R6 60 min 0-30 0-50 0-50 15-25 20-30 20-50 120 min 0-40 0-75 0-75 25-40 35-50 40-75 240 min 3-55 3-95 10-95 40-70 55-75 60-95 480 min 10-65 10-100 35-100 60-90 80-95 80-100 720 min 20-75 20-100 55-100 70-100 90-100 90-100 960 min 30-88 30-100 70-100 >80 95-100 1440 min 50-100 50-100 >90 2160 min >80 >80 Further preferred release profiles R, to R6 are summarized in the table here below [all data in wt.-% of released opioid (A)]:
time R7 R8 R9 Rip R11 R12 30 min 17.5 7.5 17.5 6.5 17.5 5.5 17.5 4.5 17.5 3.5 17.5 2.5 60 min 27.0 8.0 27.0 7.0 27.0 6.0 27.0 5.0 27.0 4.0 27.0 3.0 120 min 41.5 9.5 41.5 8.5 41.5 7.5 41.5 6.5 41.5 5.5 41.5 4.5 240 min 64.5 12.5 64.5 11.5 64.5 10.5 64.5 9.5 64.5 8.5 64.5 7.5 480 min 88.0 12.0 88.0 11.0 88.0 10.0 88.0 9.0 88.0 8.0 88.0 7.0 720 min 96.0 9.0 96.0 8.0 96.0 7.0 96.0 6.0 96.0 5.0 96.0 4.0 840 min 97.5 7.5 97.5 6.5 97.5 5.5 97.5 4.5 97.5 3.5 97.5 2.5 Preferably, the release profile of the pharmaceutical dosage form according to the present invention is stable upon storage, preferably upon storage at elevated temperature, e.g. 37 C, for 3 months in sealed containers. In this regard "stable" means that when comparing the initial release profile with the release profile after storage, at any given time point the release profiles deviate from one another by not more than 20%, more preferably not more than 15%, still more preferably not more than 10%, yet more preferably not more than 7.5%, most preferably not more than 5.0% and in particular not more than 2.5%.
Preferably, under in vitro conditions the pharmaceutical dosage form has released after 0.5 h 1.0 to 35 wt.-%, after 1 h 5.0 to 45 wt.-%, after 2 h 10 to 60 wt.-%, after 4 hat least 15 wt.-%, after 6 h at least 20 wt.-%, after 8 h at least 25 wt.-% and after 12 h at least 30 wt.-% of the opioid (A) that was originally contained in the pharmaceutical dosage form.
Suitable in vitro conditions are known to the skilled artisan. In this regard it can be referred to, e.g., the Eur. Ph. Preferably, the release profile is measured under the following conditions: Paddle apparatus equipped with sinker, 50 rpm, 37 5 C, 900 mL
simulated intestinal fluid pH 6.8 (phosphate buffer) or pH 4.5. In a preferred embodiment, to rotational speed of the paddle is increased-to 100 rpm.
In a preferred embodiment, after preferably oral administration of the pharmaceutical dosage form according to the invention, in vivo the average peak plasma level (Cmax) is on average reached after tmax 4.0 2.5 h, more preferably after tmax 4.0 2.0 h, still more preferably after tmax 4.0 1.5 h, most preferably after tmax 4.0 1.0 h and in particular after tmax 4.0 0.5 h. In another preferred embodiment, after preferably oral administration of the pharmaceutical dosage form according to the invention, in vivo the average peak plasma level (Cmax) is on average reached after tmax 5.0 2.5 h, more preferably after tmax 5.0 2.0 h, still more preferably after tmax 5.0 1.5 h, most preferably after tmax 5.0 1.0 h and in particular after tmax 5.0 0.5 h. In still another preferred embodiment, after preferably oral administration of the pharmaceutical dosage form according to the invention, in vivo the average peak plasma level (Cmax) is on average reached after tmax 6.0 2.5 h, more preferably after tmax 6.0 2.0 h, still more preferably after tmax 6.0 1.5 h, most preferably after tmax 6.0 1.0 h and in particular after tmax 6.0 0.5 h.
In a preferred embodiment, the average value for t12 after preferably oral administration of the pharmaceutical dosage form according to the invention in vivo is 4.0 2.5 h, more preferably 4.0 2.0 h, still more preferably 4.0 1.5 h, most preferably 4.0 1.0 h, and in particular 4.0 0.5 h. In another preferred embodiment, the average value for t12 after preferably oral administration of the pharmaceutical dosage form according to the invention in vivo is preferably 5.0 2.5 h, more preferably 5.0 2.0 h, still more preferably 5.0 1.5 h, most preferably 5.0 1.0 h, and in particular 5.0 0.5 h. In still another preferred embodiment, the average value for t12 after preferably oral administration of the pharmaceutical dosage form according to the invention in vivo is preferably 6.0 2.5 h, more preferably 6.0 2.0 h, still more preferably 6.0 1.5 h, most preferably 6.0 1.0 h, and in particular 6.0 0.5 h.
Preferably, the pharmaceutical dosage form according to the invention contains a coating, preferably a film-coating. Suitable coating materials are known to the skilled person. Suitable coating materials are commercially available, e.g. under the trademarks Opadry and Eudragit .
Examples of suitable materials include cellulose esters and cellulose ethers, such as methyl-cellulose (MC), hydroxypropylmethylcellulose (HPMC), hyd roxypropylcel I u lose (HPC), hyd roxyethylcel I u lose (HEC), sodium carboxymethylcellulose (Na-CMC), ethylcellulose (EC), cellulose acetate phthalate (CAP), hydroxypropylmethylcellulose phthalate (HPMCP);
poly(meth)acrylates, such as aminoalkylmethacrylate copolymers, ethylacrylate methyl-methacrylate copolymers, methacrylic acid methylmethacrylate copolymers, methacrylic acid methylmethacrylate copolymers; vinyl polymers, such as polyvinylpyrrolidone, polyvinyl-acetatephtha late, polyvinyl alcohol, polyvinylacetate; and natural film formers, such as shellack.
In a particularly preferred embodiment, the coating is water-soluble. In a preferred embodiment, the coating is based on polyvinyl alcohol, such as polyvinyl alcohol-part.
hydrolyzed, and may additionally contain polyethylene glycol, such as macrogol 3350, and/or pigments. In another preferred embodiment, the coating is based on hydroxypropylmethyl-cellulose, preferably hypromellose type 2910 having a viscosity of 3 to 15 mPas.
The coating of the pharmaceutical dosage form can increase its storage stability.
The coating can be resistant to gastric juices and dissolve as a function of the pH value of the release environment. By means of this coating, it is possible to ensure that the pharmaceutical dosage form according to the invention passes through the stomach undissolved and the active compound is only released in the intestines. The coating which is resistant to gastric juices preferably dissolves at a pH value of between 5 and 7.5.
Corresponding materials and methods for the delayed release of active compounds and for the application of coatings which are resistant to gastric juices are known to the person skilled in the art, for example from "Coated Pharmaceutical dosage forms -Fundamentals, Manufacturing Techniques, Biopharmaceutical Aspects, Test Methods and Raw Materials"
by Kurt H. Bauer, K. Lehmann, Hermann P. Osterwald, Rothgang, Gerhart, 1st edition, 1998, Medpharm Scientific Publishers.
In a preferred embodiment, the pharmaceutical dosage form according to the invention contains no substances which irritate the nasal passages and/or pharynx, i.e.
substances which, when administered via the nasal passages and/or pharynx, bring about a physical reaction which is either so unpleasant for the patient that he/she does not wish to or cannot continue administration, for example burning, or physiologically counteracts taking of the corresponding active compound, for example due to increased nasal secretion or sneezing.
Further examples of substances which irritate the nasal passages and/or pharynx are those which cause burning, itching, urge to sneeze, increased formation of secretions or a combi-nation of at least two of these stimuli. Corresponding substances and the quantities thereof which are conventionally to be used are known to the person skilled in the art. Some of the substances which irritate the nasal passages and/or pharynx are accordingly based on one or more constituents or one or more plant parts of a hot substance drug.
Corresponding hot substance drugs are known per se to the person skilled in the art and are described, for example, in "Pharmazeutische Biologie - Drogen and ihre Inhaltsstoffe" by Prof. Dr. Hildebert Wagner, 2nd., revised edition, Gustav Fischer Verlag, Stuttgart-New York, 1982, pages 82 et seq.. The corresponding description is hereby introduced as a reference and is deemed to be part of the disclosure.
The pharmaceutical dosage form according to the invention furthermore preferably contains no antagonists for the opioid (A), preferably no antagonists against psychotropic substances, in particular no antagonists against opioids (A). Antagonists suitable for a given opioid (A) are known to the person skilled in the art and may be present as such or in the form of corresponding derivatives, in particular esters or ethers, or in each case in the form of corresponding physiologically acceptable compounds, in particular in the form of the salts or solvates thereof. The pharmaceutical dosage form according to the invention preferably contains no antagonists selected from among the group comprising naloxone, naltrexone, nalmefene, nalide, nalmexone, nalorphine or naluphine, in each case optionally in the form of a corresponding physiologically acceptable compound, in particular in the form of a base, a salt or solvate; and no neuroleptics, for example a compound selected from among the group comprising haloperidol, promethacine, fluphenazine, perphenazine, levomepromazine, thiori-dazine, perazine, chlorpromazine, chlorprothixine, zuclopenthixol, flupentixol, prothipendyl, zotepine, benperidol, pipamperone, melperone and bromperidol.
The pharmaceutical dosage form according to the invention furthermore preferably contains no emetic. Emetics are known to the person skilled in the art and may be present as such or in the form of corresponding derivatives, in particular esters or ethers, or in each case in the form of corresponding physiologically acceptable compounds, in particular in the form of the salts or solvates thereof. The pharmaceutical dosage form according to the invention preferably contains no emetic based on one or more constituents of ipecacuanha (ipecac) root, for example based on the constituent emetine, as are, for example, described in "Pharmazeutische Biologie - Drogen and ihre Inhaltsstoffe" by Prof. Dr.
Hildebert Wagner, 2nd, revised edition, Gustav Fischer Verlag, Stuttgart, New York, 1982. The corresponding literature description is hereby introduced as a reference and is deemed to be part of the disclosure. The pharmaceutical dosage form according to the invention preferably also contains no apomorphine as an emetic.
Finally, the pharmaceutical dosage form according to the invention preferably also contains no bitter substance. Bitter substances and the quantities effective for use may be found in US-2003/0064099 Al, the -corresponding disclosure of which should be deemed to be the disclosure of the present application and is hereby introduced as a reference.
Examples of bitter substances are aromatic oils, such as peppermint oil, eucalyptus oil, bitter almond oil, menthol, fruit aroma substances, aroma substances from lemons, oranges, limes, grapefruit or mixtures thereof, and/or denatonium benzoate.
The pharmaceutical dosage form according to the invention accordingly preferably contains neither substances which irritate the nasal passages and/or pharynx, nor antagonists for the opioid (A), nor emetics, nor bitter substances.
The pharmaceutical dosage form according to the invention is preferably adapted for oral administration.
Typically, the pharmaceutical dosage form according to the invention assumes the form of a tablet. Preferably, the pharmaceutical dosage form is neither in film form, nor multi-particulate.
The pharmaceutical dosage form according to the invention is preferably tamper-resistant.
Preferably, tamper-resistance is achieved based on the mechanical properties of the pharmaceutical dosage form so that comminution is avoided or at least substantially impeded. According to the invention, the term comminution means the pulverization of the pharmaceutical dosage form using conventional means usually available to an abuser, for example a pestle and mortar, a hammer, a mallet or other conventional means for pulverizing under the action of force. Thus, tamper-resistance preferably means that pulverization of the pharmaceutical dosage form using conventional means is avoided or at least substantially impeded.
Preferably, the mechanical properties of the pharmaceutical dosage form according to the invention, particularly its breaking strength, substantially rely on the presence and spatial distribution of polyalkylene oxide (C), although its mere presence does typically not suffice in order to achieve said properties. The advantageous mechanical properties of the pharma-ceutical dosage form according to the invention may not automatically be achieved by simply processing opioid (A), acid (B), polyalkylene oxide (C), and optionally further excipients by means of conventional methods for the preparation of pharmaceutical dosage forms. In fact, usually suitable apparatuses must be selected for the preparation and critical processing parameters must be adjusted, particularly pressure/force, temperature and time. Thus, even if conventional apparatuses are used, the process protocols usually must be adapted in order to meet the required criteria.
The pharmaceutical dosage form according to the invention has a breaking strength of at least 300 N, preferably at least 400 N, more preferably at least 500 N, still more preferably at least 750 N, yet more preferably at least 1000 N, most preferably at least 1250 N and in particular at least 1500 N.
The "breaking strength" (resistance to crushing) of a pharmaceutical dosage form is known to the skilled person. In this regard it can be referred to, e.g., W.A. Ritschel, Die Tablette, 2.
Auflage, Editio Cantor Verlag Aulendorf, 2002; H Liebermann et al., Pharmaceutical dosage forms: Tablets, Vol. 2, Informa Healthcare; 2 edition, 1990; and Encyclopedia of Pharma-ceutical Technology, Informa Healthcare; 1 edition.
For the purpose of the specification, the breaking strength is preferably defined as the amount of force that is necessary in order to fracture the pharmaceutical dosage form breaking force). Therefore, for the purpose of the specification the pharmaceutical dosage form does preferably not exhibit the desired breaking strength when it breaks, i.e., is fractured into at least two independent parts that are separated from one another. In another preferred embodiment, however, the pharmaceutical dosage form is regarded as being broken if the force decreases by 25% (threshold value) of the highest force measured during the measurement (see below).
The pharmaceutical dosage forms according to the invention are distinguished from conventional pharmaceutical dosage forms in that, due to their breaking strength, they cannot be pulverized by the application of force with conventional means, such as for example a pestle and mortar, a hammer, a mallet or other usual means for pulverization, in particular devices developed for this purpose (tablet crushers). In this regard "pulverization"
means crumbling into small particles that would immediately release the pharmacologically active compound (A) in a suitable medium. Avoidance of pulverization virtually rules out oral or parenteral, in particular intravenous or nasal abuse.
Conventional tablets typically have a breaking strength well below 200 N in any direction of extension. The breaking strength of conventional round tablets may be estimated according to the following empirical formula: Breaking Strength [in N] = 10 x Diameter Of The Tablet [in mm]. Thus, according to said empirical formula, a round tablet having a breaking strength of at least 300 N would require a diameter of at least 30 mm). Such a tablet, however, could not be swallowed. The above empirical formula preferably does not apply to the pharmaceutical dosage forms of the invention, which are not conventional but rather special.
Further, the actual mean chewing force is about 220 N (cf., e.g., P.A.
Proeschel et al., J Dent Res, 2002, 81(7), 464-468). This means that conventional tablets having a breaking strength well below 200 N may be crushed upon spontaneous chewing, whereas the pharmaceutical dosage forms according to the invention may not.
Still further, when applying a gravitational acceleration of about 9.81 m/s2, 300 N correspond to a gravitational force of more than 30 kg, i.e. the pharmaceutical dosage forms according to the invention can preferably withstand a weight of more than 30 kg without being pulverised.
Methods for measuring the breaking strength of a pharmaceutical dosage form are known to the skilled artisan. Suitable devices are commercially available.
For example, the breaking strength (resistance to crushing) can be measured in accordance with the Eur. Ph. 5.0, 2.9.8 or 6.0, 2.09.08 "Resistance to Crushing of Tablets". The test is intended to determine, under defined conditions, the resistance to crushing of tablets, measured by the force needed to disrupt them by crushing. The apparatus consists of 2 jaws facing each other, one of which moves towards the other. The flat surfaces of the jaws are perpendicular to the direction of movement. The crushing surfaces of the jaws are flat and larger than the zone of contact with the tablet. The apparatus is calibrated using a system with a precision of 1 Newton. The tablet is placed between the jaws, taking into account, where applicable, the shape, the break-mark and the inscription; for each measurement the tablet is oriented in the same way with respect to the direction of application of the force (and the direction of extension in which the breaking strength is to be measured).
The measurement is carried out on 10 tablets, taking care that all fragments of tablets have been removed before each determination. The result is expressed as the mean, minimum and maximum values of the forces measured, all expressed in Newton.
A similar description of the breaking strength (breaking force) can be found in the USP. The breaking strength can alternatively be measured in accordance with the method described therein where it is stated that the breaking strength is the force required to cause a tablet to fail (i.e., break) in a specific plane. The tablets are generally placed between two platens, one of which moves to apply sufficient force to the tablet to cause fracture.
For conventional, round (circular cross-section) tablets, loading occurs across their diameter (sometimes referred to as diametral loading), and fracture occurs in the plane. The breaking force of tablets is commonly called- hardness in the pharmaceutical literature;
however, the use of this term is misleading. In material science, the term hardness refers to the resistance of a surface to penetration or indentation by a small probe. The term crushing strength is also frequently used to describe the resistance of tablets to the application of a compressive load.
Although this term describes the true nature of the test more accurately than does hardness, it implies that tablets are actually crushed during the test, which is often not the case.
Alternatively, the breaking strength (resistance to crushing) can be measured in accordance with WO 2005/ 016313, WO 2005/016314, and WO 2006/082099, which can be regarded as a modification of the method described in the Eur. Ph. The apparatus used for the measurement is preferably a "Zwick Z 2.5" materials tester, Finax = 2.5 kN
with a maximum draw of 1150 mm, which should be set up with one column and one spindle, a clearance behind of 100 mm and a test speed adjustable between 0.1 and 800 mm/min together with testControl software. Measurement is performed using a pressure piston with screw-in inserts and a cylinder (diameter 10 mm), a force transducer, Finax= 1 kN, diameter = 8 mm, class 0.5 from 10 N, class 1 from 2 N to ISO 7500-1, with manufacturer's test certificate M
according to DIN 55350-18 (Zwick gross force Finaz = 1.45 kN) (all apparatus from Zwick GmbH & Co. KG, Ulm, Germany) with Order No BTC-FR 2.5 TH. D09 for the tester, Order No BTC-LC 0050N. P01 for the force transducer, Order No BO 70000 S06 for the centring device.
In a preferred embodiment of the invention, the breaking strength is measured by means of a breaking strength tester e.g. Sotax , type HT100 or type HT1 (Allschwil, Switzerland). Both, the Sotax HT100 and the Sotax HT1 can measure the breaking strength according to two different measurement principles: constant speed (where the test jaw is moved at a constant speed adjustable from 5-200 mm/min) or constant force (where the test jaw increases force linearly adjustable from 5-100 N/sec). In principle, both measurement principles are suitable for measuring the breaking strength of the pharmaceutical dosage form according to the invention. Preferably, the breaking strength is measured at constant speed, preferably at a constant speed of 120 mm/min.
In a preferred embodiment, the pharmaceutical dosage form is regarded as being broken if it is fractured into at least two separate pieces.
The pharmaceutical dosage form according to the invention preferably exhibits mechanical strength over a wide temperature range, in addition to the breaking strength (resistance to crushing) optionally also sufficient hardness, impact resistance, -impact elasticity, tensile strength and/or modulus of elasticity, optionally also at low temperatures (e.g. below -24 C, below -40 C or in liquid nitrogen), for it to be virtually impossible to pulverize by spontaneous chewing, grinding in a mortar, pounding, etc. Thus, preferably, the comparatively high breaking strength of the pharmaceutical dosage form according to the invention is main-tained even at low or very low temperatures, e.g., when the pharmaceutical dosage form is initially chilled to increase its brittleness, for example to temperatures below -25 C, below -40 C or even in liquid nitrogen.
The pharmaceutical dosage form according to the invention is characterized by a certain degree of breaking strength. This does not mean that the pharmaceutical dosage form must also exhibit a certain degree of hardness. Hardness and breaking strength are different physical properties. Therefore, the tamper resistance of the pharmaceutical dosage form does not necessarily depend on the hardness of the pharmaceutical dosage form.
For instance, due to its breaking strength, impact strength, elasticity modulus and tensile strength, respectively, the pharmaceutical dosage form can preferably be deformed, e.g.
plastically, when exerting an external force, for example using a hammer, but cannot be pulverized, i.e., crumbled into a high number of fragments. In other words, the pharmaceutical dosage form according to the invention is characterized by a certain degree of breaking strength, but not necessarily also by a certain degree of form stability.
Therefore, in the meaning of the specification, a pharmaceutical dosage form that is deformed when being exposed to a force in a particular direction of extension but that does not break (plastic deformation or plastic flow) is preferably to be regarded as having the desired breaking strength in said direction of extension.
A particularly preferred embodiment of the invention relates to a tamper-resistant pharmaceutical dosage form having a breaking strength of at least 300 N and being thermoformed by hot-melt extrusion, said pharmaceutical dosage form comprising - an opioid (A) selected from the group consisting of oxymorphone, oxycodone, hydromor-phone, and the physiologically acceptable salts thereof;
- a free physiologically acceptable multicarboxylic acid (B), preferably citric acid, wherein the content of the acid (B) is within the range of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form;
an antioxidant, wherein the content of the antioxidant, preferably a-tocopherol, is within the range of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form; and a polyalkylene oxide (C) having a weight average molecular weight MW of at least 200,000 g/mol;
wherein - the opioid (A) is embedded in a matrix comprising the polyalkylene oxide (C), said matrix controlling the release of the opioid (A) from the pharmaceutical dosage form;
and - after storage for 4 weeks at 40 C and 75% rel. humidity, the content of opioid (A) amounts to at least 98.0% of its original content before storage.
The pharmaceutical dosage form according to the invention may be produced by different processes, the particularly preferred of which are explained in greater detail below. Several suitable processes have already been described in the prior art. In this regard it can be referred to, e.g., WO 2005/ 016313, WO 2005/016314, WO 2005/063214, WO
2005/102286, WO 2006/002883, WO 2006/002884, WO 2006/002886, WO 2006/082097, and WO
2006/082099.
The present invention also relates to pharmaceutical dosage forms that are obtainable by any of the processes described here below.
In general, the process for the production of the pharmaceutical dosage form according to the invention preferably comprises the following steps:
(a) mixing all ingredients;
(b) optionally pre-forming the mixture obtained from step (a), preferably by applying heat and/or force to the mixture obtained from step (a), the quantity of heat supplied preferably not being sufficient to heat the polyalkylene oxide (C) up to its softening point;
(c) hardening the mixture by applying heat and force, it being possible to supply the heat during and/or before the application of force and the quantity of heat supplied being sufficient to heat the polyalkylene oxide (C) at least up to its softening point;
(d) optionally singulating the hardened mixture;
(e) optionally shaping the pharmaceutical dosage form; and (f) optionally providing a film coating.
Heat may be supplied directly, e.g. by contact or by means of hot gas such as hot air, or with the assistance of ultrasound. Force may be applied and/or the pharmaceutical dosage form may be shaped for example by direct tabletting or with the assistance of a suitable extruder, particularly by means of a screw extruder equipped with two screws (twin-screw-extruder) or by means of a planetary gear extruder.
The final shape of the pharmaceutical dosage form may either be provided during the hardening of the mixture by applying heat and force (step (c)) or in a subsequent step (step (e)). In both cases, the mixture of all components is preferably in the plastified state, i.e.
preferably, shaping is performed at a temperature at least above the softening point of the polyalkylene oxide (C). However, extrusion at lower temperatures, e.g. ambient temperature, is also possible and may be preferred.
Shaping can be performed, e.g., by means of a tabletting press comprising die and punches of appropriate shape.
A particularly preferred process for the manufacture of the pharmaceutical dosage form of the invention involves hot-melt extrusion. In this process, the pharmaceutical dosage form according to the invention is produced by thermoforming with the assistance of an extruder, preferably without there being any observable consequent discoloration of the extrudate. It has been surprisingly found that acid (B) is capable of suppressing discoloration. In the absence of acid (B), the extrudate tends to develop beige to yellowish coloring whereas in the presence of acid (B) the extrudates are substantially colorless, i.e.
white.
This process is characterized in that a) all components are mixed, b) the resultant mixture is heated in the extruder at least up to the softening point of the polyalkylene oxide (C) and extruded through the outlet orifice of the extruder by application of force, c) the still plastic extrudate is singulated and formed into the pharmaceutical dosage form or d) the cooled and optionally reheated singulated extrudate is formed into the pharma-ceutical dosage form.
Mixing of the components according to process step a) may also proceed in the extruder.
The components may also be mixed in a mixer known to the person skilled in the art. The mixer may, for example, be a roll mixer, shaking mixer, shear mixer or compulsory mixer.
Before blending with the remaining components, polyalkylene oxide (C) is preferably provided according to the invention with an antioxidant, preferably a-tocopherol. This may proceed by mixing the two components, the polyalkylene oxide (C) and the antioxidant, preferably by dissolving or suspending the antioxidant in a highly volatile solvent and homogeneously mixing this solution or suspension with polyalkylene oxide (C) and removing the solvent by drying, preferably under an inert gas atmosphere.
The, preferably molten, mixture which has been heated in the extruder at least up to the softening point of polyalkylene oxide (C) is extruded from the extruder through a die with at least one bore.
The process according to the invention requires the use of suitable extruders, preferably screw extruders. Screw extruders which are equipped with two screws (twin-screw-extruders) are particularly preferred.
The extrusion is preferably performed so that the expansion of the strand due to extrusion is not more than 30%, i.e. that when using a die with a bore having a diameter of e.g. 6 mm, the extruded strand should have a diameter of not more than 8 mm. More preferably, the expansion of the strand is not more than 25%, still more preferably not more than 20%, most preferably not more than 15% and in particular not more than 10%.
Preferably, extrusion is performed in the absence of water, i.e., no water is added. However, traces of water (e.g., caused by atmospheric humidity) may be present.
The extruder preferably comprises at least two temperature zones, with heating of the mixture at least up to the softening point of the polyalkylene oxide (C) proceeding in the first zone, which is downstream from a feed zone and optionally mixing zone. The throughput of the mixture is preferably from 1.0 kg to 15 kg/hour. In a preferred embodiment, the throughput is from 1 to 3.5 kg/hour. In another preferred embodiment, the throughput is from 4 to 15 kg/hour.
In a preferred embodiment, the die head pressure is within the range of from 25 to 100 bar.
The die head pressure can be adjusted inter alia by die geometry, temperature profile and extrusion speed.
The die geometry or the geometry of the bores is freely selectable. The die or the bores may accordingly exhibit--a round, oblong or-oval cross-section, wherein-the round cross-section preferably has a diameter of 0.1 mm to 15 mm and the oblong cross-section preferably has a maximum lengthwise extension of 21 mm and a crosswise extension of 10 mm.
Preferably, the die or the bores have a round cross-section. The casing of the extruder used according to the invention may be heated or cooled. The corresponding temperature control, i.e.
heating or cooling, is so arranged that the mixture to be extruded exhibits at least an average temperature (product temperature) corresponding to the softening temperature of the polyalkylene oxide (C) and does not rise above a temperature at which the opioid (A) to be processed may be damaged. Preferably, the temperature of the mixture to be extruded is adjusted to below 180 C, preferably below 150 C, but at least to the softening temperature of polyalkylene oxide (C). Typical extrusion temperatures are 120 C and 130 C.
In a preferred embodiment, the extruder torque is within the range of from 30 to 95%.
Extruder torque can be adjusted inter alia by die geometry, temperature profile and extrusion speed.
After extrusion of the molten mixture and optional cooling of the extruded strand or extruded strands, the extrudates are preferably singulated. This singulation may preferably be performed by cutting up the extrudates by means of revolving or rotating knives, water jet cutters, wires, blades or with the assistance of laser cutters.
Preferably, intermediate or final storage of the optionally singulated extrudate or the final shape of the pharmaceutical dosage form according to the invention is performed under oxygen-free atmosphere which may be achieved, e.g., by means of oxygen-scavengers.
The singulated extrudate may be press-formed into tablets in order to impart the final shape to the pharmaceutical dosage form.
The application of force in the extruder onto the at least plasticized mixture is adjusted by controlling the rotational speed of the conveying device in the extruder and the geometry thereof and by dimensioning the outlet orifice in such a manner that the pressure necessary for extruding the plasticized mixture is built up in the extruder, preferably immediately prior to extrusion. The extrusion parameters which, for each particular composition, are necessary to give rise to a pharmaceutical dosage form with desired mechanical properties, may be established by simple preliminary testing.
For example but not limiting, extrusion may be performed by means of a twin-screw-extruder type ZSE 18 or ZSE27 (teistritz, Nurnberg, Germany), screw diameters of 18 or 27- mm.
Screws having eccentric ends may be used. A heatable die with a round bore having a diameter of 7, 8, or 9 mm may be used. The extrusion parameters may be adjusted e.g. to the following values: rotational speed of the screws: 120 Upm; delivery rate2 kg/h for a ZSE
18 or 8 kg/h for a ZSE27; product temperature: in front of die 125 C and behind die 135 C;
and jacket temperature: 110 C.
Preferably, extrusion is performed by means of twin-screw-extruders or planetary-gear-extruders, twin-screw extruders (co-rotating or contra-rotating) being particularly preferred.
The pharmaceutical dosage form according to the invention is preferably produced by thermoforming with the assistance of an extruder without any observable consequent discoloration of the extrudates.
The process for the preparation of the pharmaceutical dosage form according to the invention is preferably performed continuously. Preferably, the process involves the extrusion of a homogeneous mixture of all components. It is particularly advantageous if the thus obtained intermediate, e.g. the strand obtained by extrusion, exhibits uniform properties.
Particularly desirable are uniform density, uniform distribution of the active compound, uniform mechanical properties, uniform porosity, uniform appearance of the surface, etc.
Only under these circumstances the uniformity of the pharmacological properties, such as the stability of the release profile, may be ensured and the amount of rejects can be kept low.
A further aspect of the invention relates to a packaging containing a pharmaceutical dosage form according to the invention and an oxygen scavenger. Suitable packages include blister packages and bottles, such as glass bottles or bottles made from thermoplastic polymers.
Suitable oxygen scavengers are known to the skilled artisan. The oxygen scavenger can be any scavenger known in the art to scavenge oxygen. Both organic and inorganic oxygen scavengers can be used.
In one embodiment, the oxygen scavenger is any metal complex exhibiting oxygen scavenging activity. Examples include complexes containing one or more of aluminum, aluminum ferrosilicon, antimony, beryllium, calcium silicon, cerium, cobalt, gallium, hafnium, iron, magnesium alloy, nickel catalyst, selenium, silicon, silver, strontium, titanium, zinc, and/or zirconium.
In yet another embodiment, one or more elements from Group IA of the periodic table and their alloys and compounds may be used as oxygen scavengers. Examples of Group IA
elements include cesium, lithium, potassium, sodium. Further examples of inorganic oxygen scavengers include one or more of sodium azide (NaN3), sodium sulfite (Na2SO3), hydrazine, and hydroxylamine.
In one embodiment, the oxygen scavenger is an organic compound. Examples include one or more of the polyterpenes, ascorbic acid, amino polycarboxylic acid, cyclohexanedione, tetramethyl piperidone, and heterocyclic compounds with N-substituted amino groups.
Oxygen scavengers and the application thereof in pharmaceutical packaging are known to the skilled artisan. In a preferred embodiment, the oxygen scavenger is selected from the group consisting of metal-catalyzed oxidizable organic polymers and anti-oxidants. Particularly preferred are those oxygen scavengers that are able to perform in a dry environment of below 60% relative humidity, preferably below 30%
relative humidity and that are combined with a dessicant. Examples of commercially available oxygen scavengers satisfying these requirements include Pharmakeep KD10 and KD20.
It has been surprisingly found that the storage stability of the pharmaceutical dosage form can be increased when keeping the oxygen content of the atmosphere within the packaging low. Methods for packaging pharmaceutical dosage forms and the application of suitable oxygen scavengers are known to the skilled artisan. In this regard it can be referred to e.g.
D.A. Dean, Pharmaceutical Packaging Technology, Taylor & Francis, 1st ed.;
F.A. Paine et al., Packaging Pharmaceutical and Healthcare Products, Springer, 1st ed.; and O.G. Piringer et al., Plastic Packaging: Interactions with Food and Pharmaceuticals, Wiley-VCH, 2nd ed.
As far as the packaging is concerned, round bottles made from polyolefins, preferably from HDPE, are preferred. The thickness of the bottle wall is preferably at least 0.25 mm, more preferably at least 0,5 mm, otherwise the bottle may collapse.
As far as the lid of the packaging is concerned, the packaging is preferably induction or heat-sealed with an aluminium foil.
It has been surprisingly found that by selecting an appropriate shape of the packaging and sealing, the vacuum that is produced by the effect of the oxygen scavenger (underpressure of about 20,000 Pa = 2 N/cm2) can be handled without causing a collapse of the packaging.
Induction sealing (e.g. 3 seconds energy) is preferred. When sealing a 75 ml bottle having an opening with a diameter of 1 inch with aluminium foil, an underpressure of 20,000 Pa due to oxygen scavenging results in a force of about 10 N corresponding to the force that is exerted by a weight of 1 kg.
The mechanical stability of the sealing can be tested either by introducing an appropriate amount of oxygen scavenger in the bottle, sealing it and waiting for a sufficient period of time, e.g. 2 days, so that the oxygen is scavenged and an underpressure of about 20,000 Pa has been developed. Alternatively, the bottle may be sealed without any oxygen scavenger in its interior and a weight of 1 kg can be placed on the aluminium foil externally thus, simulating the force.
A further aspect of the invention relates to the use of an opioid (A) for the manufacture of the pharmaceutical dosage form as described above for the treatment of pain.
A further aspect of the invention relates to the use of a pharmaceutical dosage form as described above for avoiding or hindering the abuse of the opioid (A) contained therein.
A further aspect of the invention relates to the use of a pharmaceutical dosage form as described above for avoiding or hindering the unintentional overdose of the opioid (A) contained therein.
In this regard, the invention also relates to the use of a opioid (A) as described above and/or a polyalkylene oxide (C) as described above for the manufacture of the pharmaceutical dosage form according to the invention for the prophylaxis and/or the treatment of a disorder, thereby preventing an overdose of the opioid (A), particularly due to comminution of the pharmaceutical dosage form by mechanical action.
Further, the invention relates to a method for the prophylaxis and/or the treatment of a disorder comprising the administration of the pharmaceutical dosage form according to the invention, thereby preventing an overdose of the opioid (A), particularly due to comminution of the pharmaceutical dosage form by mechanical action. Preferably, the mechanical action is selected from the group consisting of chewing, grinding in a mortar, pounding, and using apparatuses for pulverizing conventional pharmaceutical dosage forms.
The following examples further illustrate the invention but are not to be construed as limiting its scope.
Example 1 Tablets were prepared by hot-melt extrusion of various homogeneous constituent mixtures under the following, identical extrusion conditions:
extruder type: Leistritz Extruder ZSE18PH 40D equipped with high shear screws and a die of 9 mm diameter throughput: 1.0 kg/h revolution velocity: 100 rpm barrel temperature: 100 C
extrudate temperature: 120 C
The extrudate was cut into slices of 325 mg containing about 5 mg oxymorphone hydrochloride.
The individual constituents of the extruded mixtures as well as the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.-%) decomposition products ex. further ingredient (wt.-%) wt.-%
(A) PEO PEG HPMC a-toc. oNo' oNo2 E' E2 Al 1.5 76.9 10.0 10.0 1.5 I 0.06 0.58 0.41 1.93 A2 1.5 77.5 10.0 10.0 1.0 I 0.09 0.49 0.58 1.81 A3 1.5 78.0 10.0 10.0 0.5 / 0.08 0.36 0.56 1.64 A4 1.5 78.3 10.0 10.0 0.2 I 0.08 0.26 0.63 1.51 A5 1.5 78.5 10.0 10.0 0.0 I 0.07 0.17 0.81 1.69 Bi 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 B2 1.5 .40.0 10.0 46.9 1.5 / 0.09 0.55 0.64 1.76 B3 1.5 50.0 10.0 36.9 1.5 / 0.00 0.52 0.29 1.64 B4 1.5 50.0 36.9 10.0 1.5 / 0.11 0.76 0.36 1.74 C1 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 C2 1.5 76.9 / 10.0 1.5 10.00 Lutrol F68 0.05 0.53 0.65 1.83 C3 1.5 50.0 10.0 10.0 1.5 26.90 mannitol 0.08 0.82 0.39 2.72 C4 1.5 76.9 / 10.0 1.5 10.00 carnaubawax 0.12 0.53 0.39 1.03 Di 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 D2 1.5 76.8 10.0 10.0 1.5 0.10 fumaric acid 0.05 0.48 0.52 1.70 D3 1.5 76.8 10.0 10.0 1.5 0.10 Na-EDTA 0.07 0.51 0.48 1.77 D4 1.5 76.8 10.0 10.0 1.5 0.10 citric acid 0.07 0.48 0.37 1.45 El 1.5 76.9 10.0 10.0 1.5 / 0.06 0.58 0.41 1.93 E2 1.5 76.8 10.0 10.0 1.5 0.10 citric acid 0.07 0.48 0.37 1.45 E3 1.5 76.7 10.0 10.0 1.5 0.20 citric acid 0.00 0.40 0.20 1.13 Ea - 1.5-176.4 10.0- 10:0 --- -1:5 -- _0:50 citric acid-- - -0.00 - 0.06--0:12 _ 0:17--_ _ (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities ' after extrusion, before storage 2.
after storage, amber glass bottles, plastic cap, 4 weeks, 40 C, 75% rel.
humidity The decomposition products were analyzed by HPLC-UV. The elution peak for oxymor-phone-N-oxide could not be sufficiently base-line separated from a peak of an unknown degradation product (called "UK 0.83"). Thus, both peaks were jointly integrated. It becomes evident from a comparison of examples A, to A5 that the content of oxymorphone-N-oxide before storage (oNo') is not substantially changed when the content of antioxidant a-tocopherol is decreased from 1.5 wt.-% to 1.0 wt.-%, 0.5 wt.-%, 0.2 wt.-% and even 0 wt.-%.
Upon storage (oNo2), however, the content of oxymorphone-N-oxide is proportional to the content of a-tocopherol. This is most surprising because oxymorphone-N-oxide is an oxidation product and one would expect that antioxidants usually rather suppress than support the formation of oxidation products.
Nonetheless, the complete omission of antioxidant ((x-tocopherol) has disadvantages. It could be shown by viscosity measurements that the high molecular polyethylene oxide is degraded upon extrusion and/or storage in the absence of antioxidant. It has been surpri-singly found that about 0.2 wt.-% a-tocopherol suffice in order to stabilize the polyethylene oxide; higher contents of a-tocopherol do not result in higher viscosities of the polyalkylene oxide and, thus, do not prevent PEO more pronounced from degradation. Thus, the content of antioxidant (a-tocopherol) is preferably balanced so that on the one side, the high molecular weight polyethylene oxide is sufficiently stabilized and that on the other side, the undesired formation of oxymorphone-N-oxide is kept low during storage.
Further, it becomes evident from a comparison of examples B, to B4 and examples C, to C4 that the partial replacement of the high molecular weight polyethylene oxide or the total replacement of the polyethylene glycol by an alternative plasticizer does not result in a substantial decrease of the content of undesired oxymorphone-N-oxide. This is surprising because one would expect that polyethylene oxide and polyethylene glycol are potential peroxide carriers and that a reduction thereof would result in a reduction of oxidative processes such as the oxidation of oxymorphone to oxymorphone-N-oxide.
Still further, it becomes evident from a comparison of examples D, to D5 and E, to E4 that the addition of physiologically acceptable acids, particularly citric acid, leads to a reduction of the formation of oxymorphone-N-oxide. This effect is more pronounced when the amount of acid is increased. At a concentration of 0.1 wt.-%, the effect is comparatively weak, but at a con-centration of 0.2 wt.-% the effect is stronger and is further enhanced when the concentration of citric acid is increased. Not only the amount of oxymorphone-N-oxide is decreased, but also the total amount of decomposition products, particularly of those having high HPLC
retention times.
Example 2 Tablets that had been manufactured in analogy to ex. A,, B,, C1, D, and E, above were packaged in different packaging materials and stored at 40 C and 75% rel.
humidity. The decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
w0 0 0 0 0 0 0 0 L Y M O co o 0 0 -, o CO "t E 17 M O M M co E cn 0 M 0) Co C o 0 0 0 m y y + Yco 0 0 C
0 r-- m Coo rC i O o co U) v ~n C) M It 00 ce) o 0 0 0 Y rn \ o 0 a) CC) 0 ~t 0) a N E 0 0) N N I- 0 N- 0) co co 0) 0 CO O O O
(6 L U
E ui fu 'a) Y 0 0 0` \ \0 \ \ \
0) a) C`! 0 0) CO
0N E 0 in Cn M M M Ch Cl) V M 0) 0) 0 O O O O
C
co + Y Lo 0 0 Q
CO C a) C-4 CO cq Co It co N co 0 CM C4 co M O O O O O
N
(D cu E L) C N
a) (n -0 0) Y M o 0 N cli M Co 0) CO N
O XO Cn E O O Lo c) O O co p M 0) 00) 0 O O O O O o 04 N (n U) O O O 2 O O O 2 a Q) N O o v o 0 0 0 0 N U) UC 0 co LO M to p) co E u-) r 0 r u -le CO co CO 0) W O N N N
L
E co co Y 0 CD 0 0 0 0 0 o a C O O co N Cl) M E M lf) f COO Cl) o v Cc\l )) rn co 0) 0 0 0 O. 3 a) 0) Y E o 0o 0 0 0 o a) -O y LQ C~l "I: cq 0 CO O 0 CO 4 M .
CD = N 0 N CO N co 0) 00) O .- O M N
to E M C
v LLj =2 0) E 0) x0 E o 0 0 co 0 o 0 O 't O co qq- N
CO O CD co N
O N 0) 0) ) O O O O N ~
M E
.". LC) C, Co I-O C`u M M CO CO 0) O 0) M 0 M 00) 0) O O O O O E
O
c Cl) O 0 6 M W N
0 O X c O N
-c L O
Q- L O L
O CL O Z M o 0 E o 0 CO
0 (n x >, co o E - E
0 t5 0 L Y >, X cu c y- 0 o o a) 'co o O.- E E w C) o o t It has been surprisingly found that inclusion of an oxygen scavenger in the packaging results in a further stabilization of the dosage form so that the formation of decomposition products is limited to extremely low values.
Example 3:
Tablets were manufactured as described in example 1, packed into HDPE bottles of 75 ml volume together with an oxygen scavenger combined with a desiccant (Pharmakeep 20 KD), closed with a plastic cap with induction seal.
The individual constituents of the extruded mixtures, the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.-%) decomposition products ex. (wt.-%) (A) PEO PEG HPMC a-toc. Citric acid oNo' oNo2 oNo3 E' E2 E' F, 1.5 73.8 10.0 14.0 0.2 0.5 nd nd nd nd nd 0.05 F2 1.5 77.8 10.0 10.0 0.2 0.5 nd nd Ind nd 0.05 0.10 (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities after extrusion, before storage 2: after storage, HDPE bottles, plastic cap with induction seal, oxygen scavenger, 4 weeks, 40 C, 75% rel. humidity 3 after storage, HDPE bottles, plastic cap with induction seal, oxygen scavenger, 8 weeks, 40 C, 75% rel. humidity The results reveal that the purity of the product is very high after manufacturing and that the product exhibit stable during 8 weeks storage under accelerated conditions of 40 C/75% rel.
humidity.
Example 4:
Tablets were manufactured as described in example 1 but cut into slices of 215 mg representing 5 mg or 40 mg of oxymorphone HCl, after forming the tablets were coated with about 6.5 mg each of a conventional Opadry II film-coat containing polyvinylalcohol as the film forming excipient, packed into HDPE bottles of 75 ml volume together with an oxygen scavenger combined with a desiccant (Pharmakeep 20 KD), closed with a plastic cap with induction seal.
The individual constituents of the extruded mixtures, the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.-%) decomposition products ex. (wt.-%) ffG,2~33 PEO PEG HPMC a-toc. Citric acid oNo' oNo2 E' E2 70.0 16.63 10.0 0.2 0.84 nd nd nd nd 56.8 13.56 10.0 0.2 0.84 nd nd 0.05 0.05 (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC : hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities ' = after extrusion, before storage 2: after storage, HDPE bottles, plastic cap with induction seal, oxygen scavenger, 1 month, 40 C, 75% rel. humidity Example 5:
The most preferred dosage form according to example 3 is also suitable for the stabilization of oxycodone. This could be demonstrated for a formulation containing 80 mg of oxycodone HCI manufactured analogue to example 1 but, the extrudate was cut into slices of 400 mg:
constituents (wt.-%) decomposition products ex. wt.-%
(A) PEO PEG HPMC a-toc. Citric acid oNo' oNo2 Z2 H, 20 54.3 15 10 0.2 0.5 0.06 0.07 0.22 0.13 (A): oxycodone PEO : polyethylene oxide MH, 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxycodone-N-oxide (Impurity D+E) ' : after extrusion, before storage 2: after storage, amber glass bottles, plastic cap, oxygen scavenger with desiccant (Pharmakeep 20KD) 1 month, 40 C, 75% rel. humidity Example 6:
In a single dose (40 mg oxymorphone HCI, tablets of example 4), randomized, three-way crossover study with 1 week between treatments subjects were fasted overnight and meals were served 4 and 10 hours after dosing. No water was given within 1 hour of dosing. All tablets were taken with 240 mL of water (example T).
PK samples were taken for oxymorphone and 6-OH-oxymorphone predose and up through 48 hours after dosing.
Bioequivalence was compared to Opana ER (reference R).
The results are summarized in the tables here below:
Treatment Mean SD CV
Cm,, [pg/m L] T 2147 989 46%
R 2671 1163 44%
AUCT [pg*h/m L] T 38695 13836 36%
R 38171 14652 38%
AUC [pg*h/m L] T 42575 15836 37%
R 41296 15242 37%
Point Estimate T/R Lower Limit 90% Cl Upper Limit 90% Cl Cmax 79.37 71.69 87.87 AUCT 101.98 95.17 109.29 AUC 102.24 95.48 109.48 Cl = confidence interval It becomes evident that the dosage forms according to the invention having an increased breaking strength are bioequivalent to conventional dosage forms (Opana ER ).
Example 7 Tablets were prepared under identical conditions by hot-melt extrusion of two homogeneous constituent mixtures I, and 12:
I, 12 O mor hone HCI [%] 11.1 11.1 PEO [%] 68.2 63.2 PEG [%] 10.0 15.0 HPMC Shin Etsu [%] 10.0 10.0 a-toco hero) [%] 0.2 0.2 Citric acid, anhydrous [%] 0.5 0.5 Tablet weight [mg] 360 360 PEO:PEG 6.82: 1 4.21 : 1 under the following, identical extrusion conditions:
extruder type: Leistritz Extruder type Micro 27 GL 40 D equipped with medium shear screws and a die of 8 mm diameter throughput: 10 kg/h revolution velocity: 120 rpm manufacturing time: 30 min temperature of hottest heating zone: 100 C
die temperature: 130 C.
The extrudate was cut into slices of 360 mg containing about 40 mg oxymorphone hydrochloride.
100 slices were weighed individually and the standard deviation of weight was calculated.
Slices of composition I, (PEO:PEG = 6.82:1) showed a standard deviation of 2.3 %, whereas slices of composition 12 (PEO:PEG = 4.21:1) showed a standard deviation of 1.6 % only.
It becomes evident from these comparative tests that surprisingly, the processability of the extruded mass can be improved by adjusting the ratio of PEO to PEG.
Example 8 In order to investigate if also multicarboxylic acids other than citric acid could hamper the formation of oxymorphone-N-oxide, tablets containing maleinic acid or fumaric acid were manufactured as described in example 1. For comparison, also tablets containing the inorganic salt NaH2PO4 were manufactured. The samples were stored in open dishes at 40 C and 75% relative humidity for 4 weeks.
The individual constituents of the extruded mixtures as well as the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.%) decomposition products wt.%
ex. further ingredient (wt.-%) (A) PEO PEG HPMC a-toc. oNo' oNo2 E' Y2 J, 1.5 76.0 10.0 10.0 1.5 Maleinic acid 1.0 % Ind nd 0.20 0.22 J2 1.5 76.0 10.0 10.0 1.5 Fumaric acid 1.0 % nd nd 0.17 0.30 J3 1.5 76.0 10.0 10.0 1.5 NaH2PO41.0 %* nd 0.18 0.06 0.75 (A) : oxymorphone hydrochloride PEO : polyethylene oxide MW 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol *NaH2PO4: Used in form of 1.3% of the di-hydrate oNo : oxymorphone-N-oxide (mixture) E: sum of all impurities; maleinic acid, fumaric acid and related compounds subtracted from sum of impurities after extrusion, before storage 2: after storage, open dish, 4 weeks, 40 C, 75% rel. humidity In case of maleinic and fumaric acid these compounds and for maleinic acid another related compound were detected during the purity tests as impurities (up to about 40%). Their values have been subtracted from the sum of impurities It becomes evident from a comparison of examples J, and J2 to A, and B, that the presence of maleinic and fumaric acid protected oxymorphone totally against oxidation to N-oxide and to a large extent against other degradation although the samples were stored in open dishes and not in closed bottles. These results are comparable to those obtained with citric acid (example 1, D4 and E2-E4). Samples containing NaH2PO4 (J3) exhibited protection against N-oxide formation and other degradation when compared to the formulations without any acidic compound (A, and B,) but to a less extent than the multicarboxylic acids like citric, maleinic and fumaric acid.
Example 9 In order to investigate if the presence of citric acid also protects oxidation sensitive opioids other than oxymorphone against N-oxidation, tablets containing oxycodone hydrochloride were manufactured as described in example 1.
For comparison, also tablets containing smaller amounts of a-tocopherol were manufactured.
The samples were stored in open dishes at 40 C and 75% relative humidity for 4 weeks.
The individual constituents of the extruded mixtures as well as the total amount of decomposition products before and after storage under accelerated storage conditions are summarized in the table here below:
constituents (wt.%) decomposition products ex. further ingredient (wt.%) wt.%
(A) PEO PEG HPMC a-toc. oNo' oNo2 E' E2 K, 1.5 77.0 10.0 10.0 1.5 / 0.05 0.58 0.31 1.63 K2 1.5 78.3 10.0 10.0 0.2 / 0.05 0.28 0.58 0.69 K3 1.5 76.0 10.0 10.0 1.5 Citric acid 1.0 nd nd 0.19 0.22 K4 1.5 77.3 1Ø0 1Ø0 _0.2 - Citricacid 1.0 nd- - - nd 0.18 0.23 (A) : oxycodone hydrochloride PEO : polyethylene oxide M,, 7 mio g/mol PEG : polyethylene glycol 6000 HPMC: hypromellose 100,000 Pa*s a-toc.: a-tocopherol oNo : oxycodone-N-oxide E: sum of all impurities after extrusion, before storage 2 : after storage, open dish, 4 weeks, 40 C, 75% rel. humidity These results show that citric acid protected oxycodone totally against oxidation to the N-oxide and to a large extent against other degradation although the samples were stored in open dishes rather than in closed bottles. Reducing the amount of a-tocopherol resulted in reduced degradation, when formulations were employed not containing citric acid. These results are comparable to those obtained with oxymorphone.
Claims (15)
1. A thermoformed pharmaceutical dosage form having a breaking strength of at least 300 N and comprising - an opioid (A), - a free physiologically acceptable acid (B) in an amount of from 0.001 to 5.0 wt.-%, based on the total weight of the pharmaceutical dosage form, and - a polyalkylene oxide (C) having a weight average molecular weight M w, of at least 500,000 g/mol.
2. The pharmaceutical dosage form according to claim 1, wherein the acid (B) is a multicar-boxylic acid.
3. The pharmaceutical dosage form according to claim 2, wherein the multicarboxylic acid is selected from the group consisting of maleic acid, fumaric acid, glutaric acid, malonic acid and citric acid.
4. The pharmaceutical dosage form according to any of the preceding claims, wherein the content of the acid (B) is within the range of from 0.005 to 2.5 wt.-%, based on the total weight of the pharmaceutical dosage form.
5. The pharmaceutical dosage form according to any of the preceding claims, which comprises a polyalkylene glycol, wherein the relative weight ratio of the polyalkylene oxide to the polyalkylene glycol is within the range of 4.2 ~ 2 : 1.
6. The pharmaceutical dosage form according to any of the preceding claims, which comprises an antioxidant.
7. The pharmaceutical dosage form according to claim 6, wherein the antioxidant is .alpha.-tocopherol.
8. The pharmaceutical dosage form according to claim 6 or 7, wherein the content of the antioxidant is within the range of from 0.001 to 5.0 wt.-%. based on the total weight of the pharmaceutical dosage form.
9. The pharmaceutical dosage form according to any of the preceding claims, wherein after storage for 4 weeks at 40°C and 75% rel. humidity, the content of opioid (A) amounts to at least 98.0% of its original content before storage.
10. The pharmaceutical dosage form according to any of the preceding claims, wherein the opioid (A) is embedded in a matrix comprising the polyalkylene oxide (C), said matrix controlling the release of the opioid from the pharmaceutical dosage form.
11. The pharmaceutical dosage form according to any of the preceding claims, wherein the opioid (A) is selected from the group consisting of oxymorphone, oxycodone, hydromor-phone, and the physiologically acceptable salts thereof.
12. The pharmaceutical dosage form according to any of the preceding claims, wherein the relative weight ratio of the polyalkylene oxide (C) and the opioid (A) is at least 1:1.
13. The pharmaceutical dosage form according to any of the preceding claims, which is adapted for administration once daily or twice daily.
14. The pharmaceutical dosage form according to any of the preceding claims, which has a breaking strength of at least 500 N.
15. A packaging containing a pharmaceutical dosage form according to any of claims 1 to 14 and an oxygen scavenger.
Applications Claiming Priority (3)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| EP09009480 | 2009-07-22 | ||
| EP09009480.6 | 2009-07-22 | ||
| PCT/EP2010/004460 WO2011009603A1 (en) | 2009-07-22 | 2010-07-21 | Tamper-resistant dosage form for oxidation-sensitive oploids |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| CA2767888A1 true CA2767888A1 (en) | 2011-01-27 |
| CA2767888C CA2767888C (en) | 2017-09-12 |
Family
ID=41263602
Family Applications (2)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA2767888A Expired - Fee Related CA2767888C (en) | 2009-07-22 | 2010-07-21 | Tamper-resistant dosage form for oxidation-sensitive opioids |
| CA2766172A Expired - Fee Related CA2766172C (en) | 2009-07-22 | 2010-07-21 | Oxidation-stabilized tamper-resistant dosage form |
Family Applications After (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA2766172A Expired - Fee Related CA2766172C (en) | 2009-07-22 | 2010-07-21 | Oxidation-stabilized tamper-resistant dosage form |
Country Status (26)
| Country | Link |
|---|---|
| US (7) | US20110020451A1 (en) |
| EP (4) | EP2456424B1 (en) |
| JP (2) | JP2012533586A (en) |
| KR (2) | KR101747156B1 (en) |
| CN (2) | CN102573806B (en) |
| AR (1) | AR077420A1 (en) |
| AU (2) | AU2010275754B2 (en) |
| BR (2) | BR112012001244A2 (en) |
| CA (2) | CA2767888C (en) |
| CL (2) | CL2011002970A1 (en) |
| CO (2) | CO6470798A2 (en) |
| EC (2) | ECSP12011591A (en) |
| ES (3) | ES2428938T3 (en) |
| HK (3) | HK1167810A1 (en) |
| HU (1) | HUE042987T2 (en) |
| IL (3) | IL216525A (en) |
| MX (2) | MX2012000644A (en) |
| NZ (2) | NZ596668A (en) |
| PE (2) | PE20120631A1 (en) |
| PL (2) | PL2997965T3 (en) |
| PT (1) | PT2456424E (en) |
| RU (3) | RU2555531C2 (en) |
| SI (1) | SI2456424T1 (en) |
| TW (1) | TWI473628B (en) |
| WO (2) | WO2011009604A1 (en) |
| ZA (2) | ZA201109446B (en) |
Families Citing this family (80)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US20040234602A1 (en) | 2001-09-21 | 2004-11-25 | Gina Fischer | Polymer release system |
| US20040253310A1 (en) | 2001-09-21 | 2004-12-16 | Gina Fischer | Morphine polymer release system |
| US7776314B2 (en) | 2002-06-17 | 2010-08-17 | Grunenthal Gmbh | Abuse-proofed dosage system |
| ATE495732T1 (en) | 2003-03-26 | 2011-02-15 | Egalet As | CONTROLLED RELEASE MORPHINE SYSTEM |
| DE102004032051A1 (en) | 2004-07-01 | 2006-01-19 | Grünenthal GmbH | Process for the preparation of a secured against misuse, solid dosage form |
| DE10336400A1 (en) | 2003-08-06 | 2005-03-24 | Grünenthal GmbH | Anti-abuse dosage form |
| US8075872B2 (en) | 2003-08-06 | 2011-12-13 | Gruenenthal Gmbh | Abuse-proofed dosage form |
| DE10361596A1 (en) * | 2003-12-24 | 2005-09-29 | Grünenthal GmbH | Process for producing an anti-abuse dosage form |
| US20070048228A1 (en) * | 2003-08-06 | 2007-03-01 | Elisabeth Arkenau-Maric | Abuse-proofed dosage form |
| DE102005005446A1 (en) | 2005-02-04 | 2006-08-10 | Grünenthal GmbH | Break-resistant dosage forms with sustained release |
| DE102004032103A1 (en) * | 2004-07-01 | 2006-01-19 | Grünenthal GmbH | Anti-abuse, oral dosage form |
| DE102004032049A1 (en) * | 2004-07-01 | 2006-01-19 | Grünenthal GmbH | Anti-abuse, oral dosage form |
| DE102005005449A1 (en) | 2005-02-04 | 2006-08-10 | Grünenthal GmbH | Process for producing an anti-abuse dosage form |
| DE102007011485A1 (en) | 2007-03-07 | 2008-09-11 | Grünenthal GmbH | Dosage form with more difficult abuse |
| EP2155167A2 (en) | 2007-06-04 | 2010-02-24 | Egalet A/S | Controlled release pharmaceutical compositions for prolonged effect |
| US20090108587A1 (en) * | 2007-07-10 | 2009-04-30 | Jason Matthew Mitmesser | Hybrid vertical axis wind turbine |
| US8383152B2 (en) | 2008-01-25 | 2013-02-26 | Gruenenthal Gmbh | Pharmaceutical dosage form |
| US8372432B2 (en) | 2008-03-11 | 2013-02-12 | Depomed, Inc. | Gastric retentive extended-release dosage forms comprising combinations of a non-opioid analgesic and an opioid analgesic |
| EP2262484B1 (en) | 2008-03-11 | 2013-01-23 | Depomed, Inc. | Gastric retentive extended-release dosage forms comprising combinations of a non-opioid analgesic and an opioid analgesic |
| HUE030803T2 (en) | 2008-05-09 | 2017-06-28 | Gruenenthal Gmbh | Process for the preparation of an intermediate powder formulation and a final solid dosage form under usage of a spray congealing step |
| NZ594207A (en) | 2009-02-06 | 2013-03-28 | Egalet Ltd | Immediate release composition resistant to abuse by intake of alcohol |
| NZ603579A (en) | 2009-06-24 | 2014-02-28 | Egalet Ltd | Controlled release formulations |
| RU2555531C2 (en) * | 2009-07-22 | 2015-07-10 | Грюненталь Гмбх | Misuse protected dosage form for oxidation sensitive opioids |
| KR101738369B1 (en) | 2009-07-22 | 2017-05-22 | 그뤼넨탈 게엠베하 | Hot-melt extruded controlled release dosage form |
| WO2011026125A2 (en) * | 2009-08-31 | 2011-03-03 | Depomed, Inc. | Gastric retentive pharmaceutical compositions for immediate and extended release of acetaminophen |
| US8597681B2 (en) | 2009-12-22 | 2013-12-03 | Mallinckrodt Llc | Methods of producing stabilized solid dosage pharmaceutical compositions containing morphinans |
| US9198861B2 (en) | 2009-12-22 | 2015-12-01 | Mallinckrodt Llc | Methods of producing stabilized solid dosage pharmaceutical compositions containing morphinans |
| US9579285B2 (en) * | 2010-02-03 | 2017-02-28 | Gruenenthal Gmbh | Preparation of a powdery pharmaceutical composition by means of an extruder |
| NZ700732A (en) | 2010-05-10 | 2015-08-28 | Euro Celtique Sa | Pharmaceutical compositions comprising hydromorphone and naloxone |
| EP2568965A1 (en) | 2010-05-10 | 2013-03-20 | Euro-Celtique S.A. | Combination of active loaded granules with additional actives |
| WO2011141489A1 (en) | 2010-05-10 | 2011-11-17 | Euro-Celtique S.A. | Manufacturing of active-free granules and tablets comprising the same |
| EP2611426B1 (en) * | 2010-09-02 | 2014-06-25 | Grünenthal GmbH | Tamper resistant dosage form comprising inorganic salt |
| AR082862A1 (en) | 2010-09-02 | 2013-01-16 | Gruenenthal Gmbh | ALTERATION RESISTANT DOSAGE FORM INCLUDING AN ANIONIC POLYMER |
| EP2826468A1 (en) | 2010-12-22 | 2015-01-21 | Purdue Pharma L.P. | Encased tamper resistant controlled release dosage forms |
| CN103327969A (en) | 2010-12-23 | 2013-09-25 | 普渡制药公司 | Tamper resistant solid oral dosage forms |
| US9050335B1 (en) | 2011-05-17 | 2015-06-09 | Mallinckrodt Llc | Pharmaceutical compositions for extended release of oxycodone and acetaminophen resulting in a quick onset and prolonged period of analgesia |
| US8741885B1 (en) | 2011-05-17 | 2014-06-03 | Mallinckrodt Llc | Gastric retentive extended release pharmaceutical compositions |
| US8858963B1 (en) | 2011-05-17 | 2014-10-14 | Mallinckrodt Llc | Tamper resistant composition comprising hydrocodone and acetaminophen for rapid onset and extended duration of analgesia |
| EA201400172A1 (en) | 2011-07-29 | 2014-06-30 | Грюненталь Гмбх | SUSTAINABLE TO DESTRUCTION TABLET THAT PROVIDES IMMEDIATE RELEASE OF MEDICINES |
| AR087359A1 (en) | 2011-07-29 | 2014-03-19 | Gruenenthal Gmbh | TEST ALTERATION TABLET PROVIDING IMMEDIATE RELEASE OF THE PHARMACO |
| KR20140075704A (en) * | 2011-10-06 | 2014-06-19 | 그뤼넨탈 게엠베하 | Tamper-resistant oral pharmaceutical dosage form comprising opioid agonist and opioid antagonist |
| WO2013127830A1 (en) | 2012-02-28 | 2013-09-06 | Grünenthal GmbH | Tamper-resistant pharmaceutical dosage form comprising nonionic surfactant |
| EP2819656A1 (en) | 2012-02-28 | 2015-01-07 | Grünenthal GmbH | Tamper-resistant dosage form comprising pharmacologically active compound and anionic polymer |
| MX362357B (en) * | 2012-04-18 | 2019-01-14 | Gruenenthal Gmbh | Tamper resistant and dose-dumping resistant pharmaceutical dosage form. |
| JP6067100B2 (en) | 2012-04-18 | 2017-01-25 | マリンクロッド エルエルシー | Immediate release abuse deterrent pharmaceutical composition |
| US10064945B2 (en) * | 2012-05-11 | 2018-09-04 | Gruenenthal Gmbh | Thermoformed, tamper-resistant pharmaceutical dosage form containing zinc |
| JP2015516406A (en) * | 2012-05-11 | 2015-06-11 | グリュネンタール・ゲゼルシャフト・ミト・ベシュレンクテル・ハフツング | Thermoformed tamper-resistant pharmaceutical dosage forms containing zinc |
| CA2877183A1 (en) * | 2012-07-06 | 2014-01-09 | Egalet Ltd. | Abuse deterrent pharmaceutical compositions for controlled release |
| CA2877774C (en) | 2012-07-12 | 2017-07-18 | Mallinckrodt Llc | Extended release, abuse deterrent pharmaceutical compositions |
| CA2795324C (en) * | 2012-11-09 | 2015-07-14 | Purdue Pharma | Pharmaceutical compositions comprising hydromorphone and naloxone |
| KR101840526B1 (en) | 2013-02-05 | 2018-03-20 | 퍼듀 퍼머 엘피 | Tamper resistant pharmaceutical formulations |
| AU2014230834B9 (en) | 2013-03-14 | 2017-08-31 | Fresenius Kabi Deutschland Gmbh | Injectable morphine formulations |
| CA2902346A1 (en) | 2013-03-14 | 2014-09-18 | Becton Dickinson France S.A.S. | Packaging system for oxygen-sensitive drugs |
| US10751287B2 (en) | 2013-03-15 | 2020-08-25 | Purdue Pharma L.P. | Tamper resistant pharmaceutical formulations |
| JP6255474B2 (en) | 2013-03-15 | 2017-12-27 | マリンクロッド エルエルシー | Abuse deterrent solid dosage form for immediate release with functional secant |
| AR096439A1 (en) | 2013-05-29 | 2015-12-30 | Gruenenthal Gmbh | DOSAGE METHOD RESISTING TO INDEED USE CONTAINING ONE OR MORE PARTICLES |
| JP6445537B2 (en) | 2013-05-29 | 2018-12-26 | グリュネンタール・ゲゼルシャフト・ミト・ベシュレンクテル・ハフツング | Tamper-resistant dosage forms containing one or more particles |
| EA032465B1 (en) | 2013-07-12 | 2019-05-31 | Грюненталь Гмбх | Tamper-resistant oral pharmaceutical dosage form containing ethylene-vinyl acetate polymer and process for the production thereof |
| US10195153B2 (en) | 2013-08-12 | 2019-02-05 | Pharmaceutical Manufacturing Research Services, Inc. | Extruded immediate release abuse deterrent pill |
| US9770514B2 (en) | 2013-09-03 | 2017-09-26 | ExxPharma Therapeutics LLC | Tamper-resistant pharmaceutical dosage forms |
| NZ719087A (en) | 2013-11-13 | 2017-12-22 | Euro Celtique Sa | Hydromorphone and naloxone for treatment of pain and opioid bowel dysfunction syndrome |
| AU2014356581C1 (en) | 2013-11-26 | 2020-05-28 | Grunenthal Gmbh | Preparation of a powdery pharmaceutical composition by means of cryo-milling |
| US9492444B2 (en) | 2013-12-17 | 2016-11-15 | Pharmaceutical Manufacturing Research Services, Inc. | Extruded extended release abuse deterrent pill |
| US10172797B2 (en) | 2013-12-17 | 2019-01-08 | Pharmaceutical Manufacturing Research Services, Inc. | Extruded extended release abuse deterrent pill |
| AU2015261060A1 (en) | 2014-05-12 | 2016-11-03 | Grunenthal Gmbh | Tamper resistant immediate release capsule formulation comprising Tapentadol |
| CA2949422A1 (en) | 2014-05-26 | 2015-12-03 | Grunenthal Gmbh | Multiparticles safeguarded against ethanolic dose-dumping |
| ES2963078T3 (en) | 2014-07-03 | 2024-03-25 | SpecGx LLC | Abuse-deterrent immediate-release formulations comprising non-cellulosic polysaccharides |
| CA2910865C (en) | 2014-07-15 | 2016-11-29 | Isa Odidi | Compositions and methods for reducing overdose |
| EP3169315B1 (en) | 2014-07-17 | 2020-06-24 | Pharmaceutical Manufacturing Research Services, Inc. | Immediate release abuse deterrent liquid fill dosage form |
| US20160106737A1 (en) | 2014-10-20 | 2016-04-21 | Pharmaceutical Manufacturing Research Services, Inc. | Extended Release Abuse Deterrent Liquid Fill Dosage Form |
| US20160310486A1 (en) | 2015-04-24 | 2016-10-27 | Grünenthal GmbH | Tamper-resistant fixed dose combination providing fast release of two drugs from particles and a matrix |
| US20160310428A1 (en) | 2015-04-24 | 2016-10-27 | Grunenthal Gmbh | Tamper-resistant fixed dose combination providing fast release of two drugs from different particles |
| BR112017022856A2 (en) | 2015-04-24 | 2018-07-17 | Gruenenthal Gmbh | tamper-proof fixed dose combination that provides rapid release of two drugs from particles |
| EP3285745A1 (en) | 2015-04-24 | 2018-02-28 | Grünenthal GmbH | Tamper-resistant dosage form with immediate release and resistance against solvent extraction |
| JP2018526414A (en) * | 2015-09-10 | 2018-09-13 | グリュネンタール・ゲゼルシャフト・ミト・ベシュレンクテル・ハフツング | Protection against oral overdose with abuse-inhibiting immediate release formulations |
| US20180303757A1 (en) * | 2015-10-23 | 2018-10-25 | Kashiv Pharma Llc | Enhanced abuse-deterrent formulations of oxycodone |
| WO2017184584A1 (en) * | 2016-04-19 | 2017-10-26 | Ascent Pharmaceuticals, Inc. | Stable packaging system for moisture and oxygen sensitive pharmaceutical dosage forms |
| CN110510641A (en) | 2016-08-26 | 2019-11-29 | 湖南金源新材料股份有限公司 | The method of ferric phosphate lithium cell waste material leaching lithium liquid enrichment |
| CN107777712A (en) | 2016-08-27 | 2018-03-09 | 湖南金源新材料股份有限公司 | The method and lithium carbonate product of industrial level lithium carbonate are produced with rough lithium fluoride |
| CA3112030A1 (en) | 2018-09-25 | 2020-04-02 | SpecGx LLC | Abuse deterrent immediate release capsule dosage forms |
Family Cites Families (575)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US2524855A (en) | 1950-10-10 | Process for the manufacture of | ||
| CA722109A (en) | 1965-11-23 | W. Mock Henry | Extrusion of ethylene oxide polymers | |
| US2806033A (en) | 1955-08-03 | 1957-09-10 | Lewenstein | Morphine derivative |
| US2987445A (en) * | 1958-10-10 | 1961-06-06 | Rohm & Haas | Drug composition |
| US3370035A (en) | 1961-06-23 | 1968-02-20 | Takeda Chemical Industries Ltd | Stabilization of polyalkylene oxide |
| US3332950A (en) | 1963-03-23 | 1967-07-25 | Endo Lab | 14-hydroxydihydronormorphinone derivatives |
| GB1147210A (en) | 1965-06-30 | 1969-04-02 | Eastman Kodak Co | Improvements in or relating to vitamins |
| US3652589A (en) | 1967-07-27 | 1972-03-28 | Gruenenthal Chemie | 1-(m-substituted phenyl)-2-aminomethyl cyclohexanols |
| US3806603A (en) | 1969-10-13 | 1974-04-23 | W Gaunt | Pharmaceutical carriers of plasticized dried milled particles of hydrated cooked rice endosperm |
| CH503520A (en) | 1969-12-15 | 1971-02-28 | Inventa Ag | Process for grinding granular materials, in particular plastic granulates, at low temperatures |
| DE2210071A1 (en) | 1971-03-09 | 1972-09-14 | PPG Industries Inc., Pittsburgh, Pa. (V.StA.) | Process for applying and curing a wide variety of coatings |
| US3865108A (en) | 1971-05-17 | 1975-02-11 | Ortho Pharma Corp | Expandable drug delivery device |
| US3966747A (en) | 1972-10-26 | 1976-06-29 | Bristol-Myers Company | 9-Hydroxy-6,7-benzomorphans |
| US4014965A (en) | 1972-11-24 | 1977-03-29 | The Dow Chemical Company | Process for scrapless forming of plastic articles |
| US3980766A (en) | 1973-08-13 | 1976-09-14 | West Laboratories, Inc. | Orally administered drug composition for therapy in the treatment of narcotic drug addiction |
| US3941865A (en) | 1973-12-10 | 1976-03-02 | Union Carbide Corporation | Extrusion of ethylene oxide resins |
| US4002173A (en) | 1974-07-23 | 1977-01-11 | International Paper Company | Diester crosslinked polyglucan hydrogels and reticulated sponges thereof |
| DE2530563C2 (en) | 1975-07-09 | 1986-07-24 | Bayer Ag, 5090 Leverkusen | Analgesic drugs with reduced potential for abuse |
| JPS603286B2 (en) | 1977-03-03 | 1985-01-26 | 日本化薬株式会社 | Constant-dissolution formulation |
| US4207893A (en) | 1977-08-29 | 1980-06-17 | Alza Corporation | Device using hydrophilic polymer for delivering drug to biological environment |
| US4175119A (en) | 1978-01-11 | 1979-11-20 | Porter Garry L | Composition and method to prevent accidental and intentional overdosage with psychoactive drugs |
| DE2822324C3 (en) * | 1978-05-22 | 1981-02-26 | Basf Ag, 6700 Ludwigshafen | Manufacture of vitamin E dry powder |
| US4211681A (en) | 1978-08-16 | 1980-07-08 | Union Carbide Corporation | Poly(ethylene oxide) compositions |
| US4200704A (en) * | 1978-09-28 | 1980-04-29 | Union Carbide Corporation | Controlled degradation of poly(ethylene oxide) |
| NO793297L (en) | 1978-10-19 | 1980-04-22 | Mallinckrodt Inc | PROCEDURE FOR THE MANUFACTURE OF OXYMORPHONE |
| US4258027A (en) | 1979-03-26 | 1981-03-24 | Mead Johnson & Company | Multi-fractionable tablet structure |
| US4215104A (en) | 1979-03-26 | 1980-07-29 | Mead Johnson & Company | Multi-fractionable tablet structure |
| CA1146866A (en) | 1979-07-05 | 1983-05-24 | Yamanouchi Pharmaceutical Co. Ltd. | Process for the production of sustained release pharmaceutical composition of solid medical material |
| US4353887A (en) | 1979-08-16 | 1982-10-12 | Ciba-Geigy Corporation | Divisible tablet having controlled and delayed release of the active substance |
| CH648754A5 (en) | 1979-08-16 | 1985-04-15 | Ciba Geigy Ag | Pharmaceutical slow release tablet |
| US4457933A (en) | 1980-01-24 | 1984-07-03 | Bristol-Myers Company | Prevention of analgesic abuse |
| JPS56169622A (en) | 1980-06-03 | 1981-12-26 | Kissei Pharmaceut Co Ltd | Method of making solid preparation from oily substance |
| DE3024416C2 (en) | 1980-06-28 | 1982-04-15 | Gödecke AG, 1000 Berlin | Process for the production of medicaments with sustained release of active substances |
| DE3105446A1 (en) | 1981-02-14 | 1982-09-02 | Basf Ag, 6700 Ludwigshafen | METHOD FOR PRODUCING ARALIPHATIC ALDEHYDES AND / OR AMINES |
| US4413919A (en) | 1981-10-30 | 1983-11-08 | International Business Machines Corporation | Ribbon loading system for printers |
| US4473640A (en) | 1982-06-03 | 1984-09-25 | Combie Joan D | Detection of morphine and its analogues using enzymatic hydrolysis |
| US4462941A (en) | 1982-06-10 | 1984-07-31 | The Regents Of The University Of California | Dynorphin amide analogs |
| US4427778A (en) * | 1982-06-29 | 1984-01-24 | Biochem Technology, Inc. | Enzymatic preparation of particulate cellulose for tablet making |
| US4485211A (en) | 1982-09-15 | 1984-11-27 | The B. F. Goodrich Company | Poly(glycidyl ether)block copolymers and process for their preparation |
| US4427681A (en) | 1982-09-16 | 1984-01-24 | Richardson-Vicks, Inc. | Thixotropic compositions easily convertible to pourable liquids |
| DE3246436A1 (en) | 1982-12-15 | 1984-06-20 | Alfred 9014 St.Gallen Rey | LAYING AREA WITH SOLARIUM RADIATION |
| US4529583A (en) | 1983-03-07 | 1985-07-16 | Clear Lake Development Group | Composition and method of immobilizing emetics and method of treating human beings with emetics |
| US4603143A (en) | 1983-05-02 | 1986-07-29 | Basf Corporation | Free-flowing, high density, fat soluble vitamin powders with improved stability |
| US4765989A (en) | 1983-05-11 | 1988-08-23 | Alza Corporation | Osmotic device for administering certain drugs |
| US4612008A (en) | 1983-05-11 | 1986-09-16 | Alza Corporation | Osmotic device with dual thermodynamic activity |
| US4783337A (en) | 1983-05-11 | 1988-11-08 | Alza Corporation | Osmotic system comprising plurality of members for dispensing drug |
| US5082668A (en) * | 1983-05-11 | 1992-01-21 | Alza Corporation | Controlled-release system with constant pushing source |
| US4599342A (en) | 1984-01-16 | 1986-07-08 | The Procter & Gamble Company | Pharmaceutical products providing enhanced analgesia |
| US4629621A (en) | 1984-07-23 | 1986-12-16 | Zetachron, Inc. | Erodible matrix for sustained release bioactive composition |
| AU592065B2 (en) | 1984-10-09 | 1990-01-04 | Dow Chemical Company, The | Sustained release dosage form based on highly plasticized cellulose ether gels |
| GB8507779D0 (en) | 1985-03-26 | 1985-05-01 | Fujisawa Pharmaceutical Co | Drug carrier |
| AU583639B2 (en) | 1985-06-24 | 1989-05-04 | Pitman-Moore Australia Limited | Ingestible capsules |
| EP0328775B1 (en) | 1985-06-28 | 1993-10-20 | Carrington Laboratories, Inc. | Processes for preparation of aloe products, products produced thereby and compositions thereof |
| US4992279A (en) | 1985-07-03 | 1991-02-12 | Kraft General Foods, Inc. | Sweetness inhibitor |
| US4851521A (en) | 1985-07-08 | 1989-07-25 | Fidia, S.P.A. | Esters of hyaluronic acid |
| DE3689650T2 (en) | 1985-12-17 | 1994-05-26 | United States Surgical Corp | High molecular weight bioabsorbable polymers and implants thereof. |
| US5229164A (en) | 1985-12-19 | 1993-07-20 | Capsoid Pharma Gmbh | Process for producing individually dosed administration forms |
| US4711894A (en) * | 1986-01-16 | 1987-12-08 | Henkel Corporation | Stabilized tocopherol in dry, particulate, free-flowing form |
| US4940556A (en) | 1986-01-30 | 1990-07-10 | Syntex (U.S.A.) Inc. | Method of preparing long acting formulation |
| US5198226A (en) | 1986-01-30 | 1993-03-30 | Syntex (U.S.A.) Inc. | Long acting nicardipine hydrochloride formulation |
| US4764378A (en) | 1986-02-10 | 1988-08-16 | Zetachron, Inc. | Buccal drug dosage form |
| JPS62232433A (en) | 1986-03-31 | 1987-10-12 | ユニオン、カ−バイド、コ−ポレ−シヨン | Catalyst to polymerization of alkylene oxide and polymerization |
| DE3612211A1 (en) | 1986-04-11 | 1987-10-15 | Basf Ag | CONTINUOUS TABLET METHOD |
| US4667013A (en) * | 1986-05-02 | 1987-05-19 | Union Carbide Corporation | Process for alkylene oxide polymerization |
| US4713243A (en) | 1986-06-16 | 1987-12-15 | Johnson & Johnson Products, Inc. | Bioadhesive extruded film for intra-oral drug delivery and process |
| USRE33093E (en) | 1986-06-16 | 1989-10-17 | Johnson & Johnson Consumer Products, Inc. | Bioadhesive extruded film for intra-oral drug delivery and process |
| USRE34990E (en) | 1986-08-07 | 1995-07-04 | Ciba-Geigy Corporation | Oral therapeutic system having systemic action |
| CA1335748C (en) | 1986-09-25 | 1995-05-30 | Jeffrey Lawrence Finnan | Crosslinked gelatins |
| US5227157A (en) | 1986-10-14 | 1993-07-13 | Board Of Regents, The University Of Texas System | Delivery of therapeutic agents |
| EP0277289B8 (en) | 1986-11-10 | 2003-05-21 | Biopure Corporation | Extra pure semi-synthetic blood substitute |
| US4892889A (en) * | 1986-11-18 | 1990-01-09 | Basf Corporation | Process for making a spray-dried, directly-compressible vitamin powder comprising unhydrolyzed gelatin |
| JPH0831303B2 (en) | 1986-12-01 | 1996-03-27 | オムロン株式会社 | Chip type fuse |
| ATE72111T1 (en) | 1987-01-14 | 1992-02-15 | Ciba Geigy Ag | THERAPEUTIC SYSTEM FOR POORLY SOLUBLE ACTIVE INGREDIENTS. |
| US4892778A (en) | 1987-05-27 | 1990-01-09 | Alza Corporation | Juxtaposed laminated arrangement |
| US5051261A (en) | 1987-11-24 | 1991-09-24 | Fmc Corporation | Method for preparing a solid sustained release form of a functionally active composition |
| EP0391959B1 (en) | 1987-12-17 | 1993-01-27 | The Upjohn Company | Tri-scored drug tablet |
| DE3812567A1 (en) | 1988-04-15 | 1989-10-26 | Basf Ag | METHOD FOR PRODUCING PHARMACEUTICAL MIXTURES |
| US4954346A (en) * | 1988-06-08 | 1990-09-04 | Ciba-Geigy Corporation | Orally administrable nifedipine solution in a solid light resistant dosage form |
| US4960814A (en) | 1988-06-13 | 1990-10-02 | Eastman Kodak Company | Water-dispersible polymeric compositions |
| US5350741A (en) | 1988-07-30 | 1994-09-27 | Kanji Takada | Enteric formulations of physiologically active peptides and proteins |
| JPH0249719A (en) | 1988-08-11 | 1990-02-20 | Dai Ichi Kogyo Seiyaku Co Ltd | Oil soluble-vitamin powder having readily water-dispersible and soluble performance |
| GB8820327D0 (en) * | 1988-08-26 | 1988-09-28 | May & Baker Ltd | New compositions of matter |
| DE3830353A1 (en) | 1988-09-07 | 1990-03-15 | Basf Ag | METHOD FOR THE CONTINUOUS PRODUCTION OF SOLID PHARMACEUTICAL FORMS |
| US5139790A (en) | 1988-10-14 | 1992-08-18 | Zetachron, Inc. | Low-melting moldable pharmaceutical excipient and dosage forms prepared therewith |
| US5004601A (en) | 1988-10-14 | 1991-04-02 | Zetachron, Inc. | Low-melting moldable pharmaceutical excipient and dosage forms prepared therewith |
| US4957668A (en) | 1988-12-07 | 1990-09-18 | General Motors Corporation | Ultrasonic compacting and bonding particles |
| US5190760A (en) * | 1989-07-08 | 1993-03-02 | Coopers Animal Health Limited | Solid pharmaceutical composition |
| US5169645A (en) | 1989-10-31 | 1992-12-08 | Duquesne University Of The Holy Ghost | Directly compressible granules having improved flow properties |
| US5200197A (en) | 1989-11-16 | 1993-04-06 | Alza Corporation | Contraceptive pill |
| GB8926612D0 (en) | 1989-11-24 | 1990-01-17 | Erba Farmitalia | Pharmaceutical compositions |
| EP0449775A3 (en) | 1990-03-29 | 1992-09-02 | Ciba-Geigy Ag | Polyether-polyester block copolymers and their use as dispersing agents |
| SU1759445A1 (en) | 1990-06-15 | 1992-09-07 | Ленинградский Технологический Институт Им.Ленсовета | Method of producing encapsulated hydrophobic substances |
| FR2664851B1 (en) | 1990-07-20 | 1992-10-16 | Oreal | METHOD OF COMPACTING A POWDER MIXTURE FOR OBTAINING A COMPACT ABSORBENT OR PARTIALLY DELITABLE PRODUCT AND PRODUCT OBTAINED BY THIS PROCESS. |
| US5125151A (en) | 1990-08-08 | 1992-06-30 | Emhart Inc. | Rivet setting tool |
| EP0477135A1 (en) | 1990-09-07 | 1992-03-25 | Warner-Lambert Company | Chewable spheroidal coated microcapsules and methods for preparing same |
| US5126151A (en) * | 1991-01-24 | 1992-06-30 | Warner-Lambert Company | Encapsulation matrix |
| US5273758A (en) | 1991-03-18 | 1993-12-28 | Sandoz Ltd. | Directly compressible polyethylene oxide vehicle for preparing therapeutic dosage forms |
| US5149538A (en) | 1991-06-14 | 1992-09-22 | Warner-Lambert Company | Misuse-resistive transdermal opioid dosage form |
| JP3073054B2 (en) | 1991-07-11 | 2000-08-07 | 住友精化株式会社 | Method for producing alkylene oxide polymer |
| WO1993004670A1 (en) | 1991-08-30 | 1993-03-18 | Showa Yakuhin Kako Co., Ltd. | Dry gel composition |
| DE69229881T2 (en) | 1991-10-04 | 1999-12-09 | Yoshitomi Pharmaceutical | DELAYED RELEASE TABLET |
| WO1993006723A1 (en) | 1991-10-04 | 1993-04-15 | Olin Corporation | Fungicide tablet |
| DE4138513A1 (en) | 1991-11-23 | 1993-05-27 | Basf Ag | SOLID PHARMACEUTICAL RETARD FORM |
| US5266331A (en) | 1991-11-27 | 1993-11-30 | Euroceltique, S.A. | Controlled release oxycodone compositions |
| ATE140620T1 (en) | 1991-12-05 | 1996-08-15 | Mallinckrodt Veterinary Inc | GLASSY CARBOHYDRATE MATRICE FOR ADMINISTRATION OF DELAYED RELEASE MEDICATIONS |
| US5200194A (en) | 1991-12-18 | 1993-04-06 | Alza Corporation | Oral osmotic device |
| EP0617612B1 (en) | 1991-12-18 | 1997-09-10 | Warner-Lambert Company | A process for the preparation of a solid dispersion |
| US5225417A (en) * | 1992-01-21 | 1993-07-06 | G. D. Searle & Co. | Opioid agonist compounds |
| IL105553A (en) | 1992-05-06 | 1998-01-04 | Janssen Pharmaceutica Inc | Solid dosage form comprising a porous network of matrix forming material which disperses rapidly in water |
| AU4316393A (en) | 1992-05-22 | 1993-12-30 | Godecke Aktiengesellschaft | Process for preparing delayed-action medicinal compositions |
| GB9217295D0 (en) | 1992-08-14 | 1992-09-30 | Wellcome Found | Controlled released tablets |
| DE4227385A1 (en) | 1992-08-19 | 1994-02-24 | Kali Chemie Pharma Gmbh | Pancreatin micropellets |
| DE4229085C2 (en) | 1992-09-01 | 1996-07-11 | Boehringer Mannheim Gmbh | Elongated, divisible tablet |
| AU682827B2 (en) | 1992-09-18 | 1997-10-23 | Astellas Pharma Inc. | Sustained-release hydrogel preparation |
| US5472943A (en) | 1992-09-21 | 1995-12-05 | Albert Einstein College Of Medicine Of Yeshiva University, | Method of simultaneously enhancing analgesic potency and attenuating dependence liability caused by morphine and other opioid agonists |
| FI101039B (en) | 1992-10-09 | 1998-04-15 | Eeva Kristoffersson | Method for preparing medicated pellets |
| AU679937B2 (en) | 1992-11-18 | 1997-07-17 | Johnson & Johnson Consumer Products, Inc. | Extrudable compositions for topical or transdermal drug delivery |
| JP3459421B2 (en) | 1992-12-23 | 2003-10-20 | サイテック ソチエタ レスポンサビリタ リミテ | Process for the preparation of controlled open pharmaceutical forms and the pharmaceutical forms thus obtained |
| GB2273874A (en) | 1992-12-31 | 1994-07-06 | Pertti Olavi Toermaelae | Preparation of pharmaceuticals in a polymer matrix |
| US6071970A (en) | 1993-02-08 | 2000-06-06 | Nps Pharmaceuticals, Inc. | Compounds active at a novel site on receptor-operated calcium channels useful for treatment of neurological disorders and diseases |
| US5914132A (en) | 1993-02-26 | 1999-06-22 | The Procter & Gamble Company | Pharmaceutical dosage form with multiple enteric polymer coatings for colonic delivery |
| DE4309528C2 (en) | 1993-03-24 | 1998-05-20 | Doxa Gmbh | Casein film or film tube, process for their production and their use |
| IL119660A (en) | 1993-05-10 | 2002-09-12 | Euro Celtique Sa | Controlled release formulation comprising tramadol |
| IL109944A (en) | 1993-07-01 | 1998-12-06 | Euro Celtique Sa | Sustained release dosage unit forms containing morphine and a method of preparing these sustained release dosage unit forms |
| DE4329794C2 (en) | 1993-09-03 | 1997-09-18 | Gruenenthal Gmbh | Tramadol salt-containing drugs with delayed release |
| EP0647448A1 (en) | 1993-10-07 | 1995-04-12 | Euroceltique S.A. | Orally administrable opioid formulations having extended duration of effect |
| KR100354702B1 (en) | 1993-11-23 | 2002-12-28 | 유로-셀티크 소시에떼 아노뉨 | Manufacturing method and sustained release composition of pharmaceutical composition |
| ES2168290T3 (en) | 1993-11-23 | 2002-06-16 | Euro Celtique Sa | METHOD FOR PREPARING A SUSTAINED RELEASE COMPOSITION. |
| WO1995017174A1 (en) | 1993-12-20 | 1995-06-29 | The Procter & Gamble Company | Process for making laxatives containing dioctyl sulfosuccinate |
| IL112106A0 (en) * | 1993-12-22 | 1995-03-15 | Ergo Science Inc | Accelerated release composition containing bromocriptine |
| GB9401894D0 (en) | 1994-02-01 | 1994-03-30 | Rhone Poulenc Rorer Ltd | New compositions of matter |
| CA2182282C (en) | 1994-02-16 | 2006-04-18 | Jacqueline E. Briskin | Process for preparing fine particle pharmaceutical formulations |
| SE9503924D0 (en) * | 1995-08-18 | 1995-11-07 | Astra Ab | Novel opioid peptides |
| US5458887A (en) | 1994-03-02 | 1995-10-17 | Andrx Pharmaceuticals, Inc. | Controlled release tablet formulation |
| DE4413350A1 (en) | 1994-04-18 | 1995-10-19 | Basf Ag | Retard matrix pellets and process for their production |
| JP2977907B2 (en) | 1994-05-06 | 1999-11-15 | ファイザー・インコーポレーテッド | Controlled release dosage form of azithromycin |
| DE19509807A1 (en) * | 1995-03-21 | 1996-09-26 | Basf Ag | Process for the preparation of active substance preparations in the form of a solid solution of the active substance in a polymer matrix, and active substance preparations produced using this method |
| AT403988B (en) | 1994-05-18 | 1998-07-27 | Lannacher Heilmittel | SOLID ORAL RETARDED PREPARATION |
| US5460826A (en) | 1994-06-27 | 1995-10-24 | Alza Corporation | Morphine therapy |
| DE4426245A1 (en) | 1994-07-23 | 1996-02-22 | Gruenenthal Gmbh | 1-phenyl-3-dimethylamino-propane compounds with pharmacological activity |
| IT1274879B (en) | 1994-08-03 | 1997-07-25 | Saitec Srl | APPARATUS AND METHOD FOR PREPARING SOLID PHARMACEUTICAL FORMS WITH CONTROLLED RELEASE OF THE ACTIVE INGREDIENT. |
| JPH0851331A (en) | 1994-08-04 | 1996-02-20 | Asahi Kasei Micro Syst Kk | Automatic gain control circuit |
| JP3285452B2 (en) | 1994-08-11 | 2002-05-27 | サンスター株式会社 | Toothpaste composition |
| US5837790A (en) * | 1994-10-24 | 1998-11-17 | Amcol International Corporation | Precipitation polymerization process for producing an oil adsorbent polymer capable of entrapping solid particles and liquids and the product thereof |
| AUPM897594A0 (en) | 1994-10-25 | 1994-11-17 | Daratech Pty Ltd | Controlled release container |
| US5965161A (en) | 1994-11-04 | 1999-10-12 | Euro-Celtique, S.A. | Extruded multi-particulates |
| DE4446470A1 (en) | 1994-12-23 | 1996-06-27 | Basf Ag | Process for the production of dividable tablets |
| DE19504832A1 (en) | 1995-02-14 | 1996-08-22 | Basf Ag | Solid drug preparations |
| US5945125A (en) | 1995-02-28 | 1999-08-31 | Temple University | Controlled release tablet |
| US6348469B1 (en) * | 1995-04-14 | 2002-02-19 | Pharma Pass Llc | Solid compositions containing glipizide and polyethylene oxide |
| US6117453A (en) | 1995-04-14 | 2000-09-12 | Pharma Pass | Solid compositions containing polyethylene oxide and an active ingredient |
| US5900425A (en) | 1995-05-02 | 1999-05-04 | Bayer Aktiengesellschaft | Pharmaceutical preparations having controlled release of active compound and processes for their preparation |
| DE19522899C1 (en) | 1995-06-23 | 1996-12-19 | Hexal Pharmaforschung Gmbh | Process for the continuous sintering of a granulate |
| US5759583A (en) | 1995-08-30 | 1998-06-02 | Syntex (U.S.A.) Inc. | Sustained release poly (lactic/glycolic) matrices |
| US7590224B1 (en) * | 1995-09-15 | 2009-09-15 | At&T Intellectual Property, Ii, L.P. | Automated task classification system |
| US6063405A (en) | 1995-09-29 | 2000-05-16 | L.A.M. Pharmaceuticals, Llc | Sustained release delivery system |
| US5811126A (en) | 1995-10-02 | 1998-09-22 | Euro-Celtique, S.A. | Controlled release matrix for pharmaceuticals |
| DE19539361A1 (en) | 1995-10-23 | 1997-04-24 | Basf Ag | Process for the preparation of multilayer, solid pharmaceutical forms for oral or rectal administration |
| US6096330A (en) | 1995-11-22 | 2000-08-01 | The Secretary Of State For Minister Of Agriculture Fisheries & Food In Her Britannic Majesty's Government Of The United Kingdom Of Great Britain And Northern Ireland | Alkylphosphines as pesticidal agents |
| US6355656B1 (en) * | 1995-12-04 | 2002-03-12 | Celgene Corporation | Phenidate drug formulations having diminished abuse potential |
| US5908850A (en) * | 1995-12-04 | 1999-06-01 | Celgene Corporation | Method of treating attention deficit disorders with d-threo methylphenidate |
| DE19547766A1 (en) | 1995-12-20 | 1997-06-26 | Gruenenthal Gmbh | 1-phenyl-2-dimethylaminomethyl-cyclohexan-1-ol compounds as active pharmaceutical ingredients |
| ES2168610T3 (en) | 1996-03-12 | 2002-06-16 | Alza Corp | COMPOSITION AND GALENIC FORM CONTAINING AN OPIOID ANTAGONIST. |
| US6461644B1 (en) | 1996-03-25 | 2002-10-08 | Richard R. Jackson | Anesthetizing plastics, drug delivery plastics, and related medical products, systems and methods |
| EP0914158B2 (en) | 1996-04-05 | 2006-01-25 | Takeda Chemical Industries, Ltd. | Pharmaceutical combination containing a compound having angiotensin ii antagonistic activity and a compound which increases the insulin-sensitivity |
| US6096339A (en) | 1997-04-04 | 2000-08-01 | Alza Corporation | Dosage form, process of making and using same |
| US20020114838A1 (en) | 1996-04-05 | 2002-08-22 | Ayer Atul D. | Uniform drug delivery therapy |
| US5817343A (en) * | 1996-05-14 | 1998-10-06 | Alkermes, Inc. | Method for fabricating polymer-based controlled-release devices |
| US6455052B1 (en) | 1996-06-06 | 2002-09-24 | Bifodan A/S | Enteric coating, comprising alginic acid, for an oral preparation |
| DE09003265T1 (en) | 1996-06-26 | 2010-04-29 | Board of Regents, The University of Texas System, Austin | Extrudable pharmaceutical hot melt adhesive formulation |
| WO1998001117A1 (en) | 1996-07-08 | 1998-01-15 | Edward Mendell Co., Inc. | Sustained release matrix for high-dose insoluble drugs |
| DE19629753A1 (en) * | 1996-07-23 | 1998-01-29 | Basf Ag | Process for the production of solid dosage forms |
| NL1003684C2 (en) | 1996-07-25 | 1998-01-28 | Weterings B V H | Device for dispensing a liquid. |
| DE19630236A1 (en) | 1996-07-26 | 1998-01-29 | Wolff Walsrode Ag | Biaxially stretched, biodegradable and compostable sausage casing |
| BE1010353A5 (en) | 1996-08-14 | 1998-06-02 | Boss Pharmaceuticals Ag | Method for manufacture of pharmaceutical products, device for such a method and pharmaceutical products obtained. |
| JP4034357B2 (en) | 1996-11-05 | 2008-01-16 | ノバモント・ソシエタ・ペル・アチオニ | Biodegradable polymer composition comprising starch and thermoplastic polymer |
| US5991799A (en) | 1996-12-20 | 1999-11-23 | Liberate Technologies | Information retrieval system using an internet multiplexer to focus user selection |
| DE19705538C1 (en) | 1997-02-14 | 1998-08-27 | Goedecke Ag | Process for the separation of active substances in solid pharmaceutical preparations |
| US5948787A (en) | 1997-02-28 | 1999-09-07 | Alza Corporation | Compositions containing opiate analgesics |
| DE19710008A1 (en) | 1997-03-12 | 1998-09-17 | Basf Ag | Solid, at least two-phase formulations of a sustained-release opioid analgesic |
| DE19710009A1 (en) | 1997-03-12 | 1998-09-24 | Knoll Ag | Multi-phase preparation forms containing active ingredients |
| DE19710213A1 (en) | 1997-03-12 | 1998-09-17 | Basf Ag | Process for the manufacture of solid combination dosage forms |
| US6139770A (en) | 1997-05-16 | 2000-10-31 | Chevron Chemical Company Llc | Photoinitiators and oxygen scavenging compositions |
| DE19721467A1 (en) | 1997-05-22 | 1998-11-26 | Basf Ag | Process for the preparation of small-scale preparations of biologically active substances |
| US6635280B2 (en) | 1997-06-06 | 2003-10-21 | Depomed, Inc. | Extending the duration of drug release within the stomach during the fed mode |
| EP0998271B3 (en) | 1997-06-06 | 2014-10-29 | Depomed, Inc. | Gastric-retentive oral drug dosage forms for controlled release of highly soluble drugs |
| DK1009387T3 (en) | 1997-07-02 | 2006-08-14 | Euro Celtique Sa | Long-release stabilized tramadol formulations |
| IE970588A1 (en) * | 1997-08-01 | 2000-08-23 | Elan Corp Plc | Controlled release pharmaceutical compositions containing tiagabine |
| AU741599B2 (en) | 1997-09-10 | 2001-12-06 | Fram Group Ip Llc | Injection molding of structural zirconia-based materials by an aqueous process |
| US6009390A (en) | 1997-09-11 | 1999-12-28 | Lucent Technologies Inc. | Technique for selective use of Gaussian kernels and mixture component weights of tied-mixture hidden Markov models for speech recognition |
| PT1033975E (en) | 1997-11-28 | 2002-07-31 | Knoll Ag | PROCESS FOR THE PREPARATION OF BIOLOGICALLY ACTIVE NAO-CRYSTALLINE SUBSTANCES ISSUED OF DISSOLVENTS |
| CN1278839A (en) | 1997-12-03 | 2001-01-03 | 拜尔公司 | Polyether ester amides |
| DE19753534A1 (en) | 1997-12-03 | 1999-06-10 | Bayer Ag | Biodegradable thermoplastic polyester-amides with good mechanical properties for molding, film and fiber, useful for e.g. compostable refuse bag |
| US6375957B1 (en) * | 1997-12-22 | 2002-04-23 | Euro-Celtique, S.A. | Opioid agonist/opioid antagonist/acetaminophen combinations |
| CA2314896C (en) | 1997-12-22 | 2005-09-13 | Euro-Celtique, S.A. | A method of preventing abuse of opioid dosage forms |
| DE19800698A1 (en) | 1998-01-10 | 1999-07-15 | Bayer Ag | Biodegradable polyester amides with block-like polyester and polyamide segments |
| DE19800689C1 (en) | 1998-01-10 | 1999-07-15 | Deloro Stellite Gmbh | Shaped body made of a wear-resistant material |
| US6251430B1 (en) | 1998-02-04 | 2001-06-26 | Guohua Zhang | Water insoluble polymer based sustained release formulation |
| EP1045885A1 (en) | 1998-02-06 | 2000-10-25 | Union Carbide Chemicals & Plastics Technology Corporation | Alkylene oxide polymer compositions |
| EP0980894B1 (en) | 1998-03-05 | 2004-06-23 | Mitsui Chemicals, Inc. | Polylactic acid composition and film thereof |
| US6245357B1 (en) | 1998-03-06 | 2001-06-12 | Alza Corporation | Extended release dosage form |
| US6090411A (en) | 1998-03-09 | 2000-07-18 | Temple University | Monolithic tablet for controlled drug release |
| US6110500A (en) | 1998-03-25 | 2000-08-29 | Temple University | Coated tablet with long term parabolic and zero-order release kinetics |
| JP2002510878A (en) * | 1998-04-02 | 2002-04-09 | アプライド マテリアルズ インコーポレイテッド | Method for etching a low-k dielectric |
| CA2327685C (en) | 1998-04-03 | 2008-11-18 | Bm Research A/S | Controlled release composition |
| US5962488A (en) * | 1998-04-08 | 1999-10-05 | Roberts Laboratories, Inc. | Stable pharmaceutical formulations for treating internal bowel syndrome containing isoxazole derivatives |
| DE19822979A1 (en) | 1998-05-25 | 1999-12-02 | Kalle Nalo Gmbh & Co Kg | Film with starch or starch derivatives and polyester urethanes and process for their production |
| US6333087B1 (en) * | 1998-08-27 | 2001-12-25 | Chevron Chemical Company Llc | Oxygen scavenging packaging |
| DE19841244A1 (en) | 1998-09-09 | 2000-03-16 | Knoll Ag | Method and device for making tablets |
| GT199900148A (en) | 1998-09-10 | 2001-02-28 | Denaturing for the sympathomimetic amine salts. | |
| US6268177B1 (en) | 1998-09-22 | 2001-07-31 | Smithkline Beecham Corporation | Isolated nucleic acid encoding nucleotide pyrophosphorylase |
| WO2000023073A1 (en) | 1998-10-20 | 2000-04-27 | Korea Institute Of Science And Technology | Bioflavonoids as plasma high density lipoprotein level increasing agent |
| US6322819B1 (en) | 1998-10-21 | 2001-11-27 | Shire Laboratories, Inc. | Oral pulsed dose drug delivery system |
| US20060240105A1 (en) | 1998-11-02 | 2006-10-26 | Elan Corporation, Plc | Multiparticulate modified release composition |
| ES2141688B1 (en) | 1998-11-06 | 2001-02-01 | Vita Invest Sa | NEW ESTERS DERIVED FROM SUBSTITUTED FENIL-CICLOHEXIL COMPOUNDS. |
| DE19855440A1 (en) | 1998-12-01 | 2000-06-08 | Basf Ag | Process for the production of solid dosage forms by melt extrusion |
| DE19856147A1 (en) | 1998-12-04 | 2000-06-08 | Knoll Ag | Divisible solid dosage forms and methods for their preparation |
| EP1005863A1 (en) | 1998-12-04 | 2000-06-07 | Synthelabo | Controlled-release dosage forms comprising a short acting hypnotic or a salt thereof |
| US6238697B1 (en) | 1998-12-21 | 2001-05-29 | Pharmalogix, Inc. | Methods and formulations for making bupropion hydrochloride tablets using direct compression |
| WO2000040205A2 (en) | 1999-01-05 | 2000-07-13 | Copley Pharmaceutical Inc. | Sustained release formulation with reduced moisture sensitivity |
| WO2000045830A1 (en) | 1999-02-04 | 2000-08-10 | Nichimo Co., Ltd. | Materials for preventing arteriosclerosis, immunopotentiating materials, vertebrates fed with these materials and eggs thereof |
| US7374779B2 (en) * | 1999-02-26 | 2008-05-20 | Lipocine, Inc. | Pharmaceutical formulations and systems for improved absorption and multistage release of active agents |
| US6375963B1 (en) * | 1999-06-16 | 2002-04-23 | Michael A. Repka | Bioadhesive hot-melt extruded film for topical and mucosal adhesion applications and drug delivery and process for preparation thereof |
| US6384020B1 (en) | 1999-07-14 | 2002-05-07 | Shire Laboratories, Inc. | Rapid immediate release oral dosage form |
| US20030118641A1 (en) | 2000-07-27 | 2003-06-26 | Roxane Laboratories, Inc. | Abuse-resistant sustained-release opioid formulation |
| MXPA02000725A (en) | 1999-07-29 | 2003-07-14 | Roxane Lab Inc | Opioid sustained released formulation. |
| US6562375B1 (en) * | 1999-08-04 | 2003-05-13 | Yamanouchi Pharmaceuticals, Co., Ltd. | Stable pharmaceutical composition for oral use |
| PT1205190E (en) | 1999-08-04 | 2006-09-29 | Astellas Pharma Inc | MEDICINAL COMPOSITIONS STABLE FOR ORAL USE USING IRON OXIDES |
| KR100345214B1 (en) | 1999-08-17 | 2002-07-25 | 이강춘 | The nasal transmucosal delivery of peptides conjugated with biocompatible polymers |
| DE19940740A1 (en) * | 1999-08-31 | 2001-03-01 | Gruenenthal Gmbh | Pharmaceutical salts |
| ATE279186T1 (en) | 1999-08-31 | 2004-10-15 | Gruenenthal Gmbh | SUSTAINED-RELEASE PHARMACEUTICAL FORM CONTAINING TRAMADOL ACCHARINATE |
| DE19940944B4 (en) | 1999-08-31 | 2006-10-12 | Grünenthal GmbH | Retarded, oral, pharmaceutical dosage forms |
| DE19960494A1 (en) | 1999-12-15 | 2001-06-21 | Knoll Ag | Device and method for producing solid active substance-containing forms |
| ES2160534B1 (en) | 1999-12-30 | 2002-04-16 | Vita Invest Sa | NEW ESTERS DERIVED FROM (RR, SS) -2-HYDROXIBENZOATE 3- (2-DIMETHYLMINOME-1-HYDROXICICLOHEXIL) PHENYL. |
| US6680070B1 (en) | 2000-01-18 | 2004-01-20 | Albemarle Corporation | Particulate blends and compacted products formed therefrom, and the preparation thereof |
| HUP0204163A2 (en) | 2000-02-08 | 2003-04-28 | Euro-Celtique S.A. | Controlled-release composition containing opioid agonist and antagonist and process for its preparation |
| US20020015730A1 (en) | 2000-03-09 | 2002-02-07 | Torsten Hoffmann | Pharmaceutical formulations and method for making |
| DE10015479A1 (en) | 2000-03-29 | 2001-10-11 | Basf Ag | Solid oral dosage forms with delayed release of active ingredient and high mechanical stability |
| US8012504B2 (en) | 2000-04-28 | 2011-09-06 | Reckitt Benckiser Inc. | Sustained release of guaifenesin combination drugs |
| US6572887B2 (en) | 2000-05-01 | 2003-06-03 | National Starch And Chemical Investment Holding Corporation | Polysaccharide material for direct compression |
| US6419954B1 (en) | 2000-05-19 | 2002-07-16 | Yamanouchi Pharmaceutical Co., Ltd. | Tablets and methods for modified release of hydrophilic and other active agents |
| CA2409996C (en) | 2000-05-23 | 2016-03-01 | Cenes Pharmaceuticals, Inc. | Nrg-2 nucleic acid molecules, polypeptides, and diagnostic and therapeutic methods |
| DE10029201A1 (en) | 2000-06-19 | 2001-12-20 | Basf Ag | Retarded release oral dosage form, obtained by granulating mixture containing active agent and polyvinyl acetate-polyvinyl pyrrolidone mixture below the melting temperature |
| US6488962B1 (en) | 2000-06-20 | 2002-12-03 | Depomed, Inc. | Tablet shapes to enhance gastric retention of swellable controlled-release oral dosage forms |
| US6607748B1 (en) | 2000-06-29 | 2003-08-19 | Vincent Lenaerts | Cross-linked high amylose starch for use in controlled-release pharmaceutical formulations and processes for its manufacture |
| DE10036400A1 (en) | 2000-07-26 | 2002-06-06 | Mitsubishi Polyester Film Gmbh | White, biaxially oriented polyester film |
| US6642205B2 (en) | 2000-09-25 | 2003-11-04 | Pro-Pharmaceuticals, Inc. | Methods and compositions for reducing side effects in chemotherapeutic treatments |
| WO2002026061A1 (en) | 2000-09-27 | 2002-04-04 | Danisco A/S | Antimicrobial agent |
| WO2002026928A1 (en) | 2000-09-28 | 2002-04-04 | The Dow Chemical Company | Polymer composite structures useful for controlled release systems |
| GB0026137D0 (en) | 2000-10-25 | 2000-12-13 | Euro Celtique Sa | Transdermal dosage form |
| US6344215B1 (en) | 2000-10-27 | 2002-02-05 | Eurand America, Inc. | Methylphenidate modified release formulations |
| AU2738302A (en) | 2000-10-30 | 2002-05-15 | Euro Celtique Sa | Controlled release hydrocodone formulations |
| AU2002226098A1 (en) | 2000-10-30 | 2002-05-15 | The Board Of Regents, The University Of Texas System | Spherical particles produced by a hot-melt extrusion/spheronization process |
| DE10109763A1 (en) | 2001-02-28 | 2002-09-05 | Gruenenthal Gmbh | Pharmaceutical salts |
| JP2002265592A (en) | 2001-03-07 | 2002-09-18 | Sumitomo Seika Chem Co Ltd | Process for producing alkylene oxide polymer |
| WO2002071860A1 (en) | 2001-03-13 | 2002-09-19 | L.A. Dreyfus Co. | Gum base and gum manufacturing using particulated gum base ingredients |
| JP3967554B2 (en) | 2001-03-15 | 2007-08-29 | 株式会社ポッカコーポレーション | Flavonoid compound and method for producing the same |
| US20020132395A1 (en) * | 2001-03-16 | 2002-09-19 | International Business Machines Corporation | Body contact in SOI devices by electrically weakening the oxide under the body |
| EP1241110A1 (en) * | 2001-03-16 | 2002-09-18 | Pfizer Products Inc. | Dispensing unit for oxygen-sensitive drugs |
| EP1385486A4 (en) | 2001-04-18 | 2006-05-17 | Nostrum Pharmaceuticals Inc | A novel coating for a sustained release pharmaceutical composition |
| US20020187192A1 (en) | 2001-04-30 | 2002-12-12 | Yatindra Joshi | Pharmaceutical composition which reduces or eliminates drug abuse potential |
| EP1385898B1 (en) | 2001-05-01 | 2006-05-31 | Union Carbide Chemicals & Plastics Technology Corporation | Pharmaceutical composition comprising poly(alkylene oxides) having reduced amounts of formic compounds |
| UA81224C2 (en) | 2001-05-02 | 2007-12-25 | Euro Celtic S A | Dosage form of oxycodone and use thereof |
| WO2002090316A1 (en) | 2001-05-08 | 2002-11-14 | The Johns Hopkins University | Method of inhibiting methamphetamine synthesis |
| US20030065002A1 (en) | 2001-05-11 | 2003-04-03 | Endo Pharmaceuticals, Inc. | Abuse-resistant controlled-release opioid dosage form |
| US6623754B2 (en) | 2001-05-21 | 2003-09-23 | Noveon Ip Holdings Corp. | Dosage form of N-acetyl cysteine |
| US7125561B2 (en) | 2001-05-22 | 2006-10-24 | Euro-Celtique S.A. | Compartmentalized dosage form |
| US20030064122A1 (en) | 2001-05-23 | 2003-04-03 | Endo Pharmaceuticals, Inc. | Abuse resistant pharmaceutical composition containing capsaicin |
| US7968119B2 (en) | 2001-06-26 | 2011-06-28 | Farrell John J | Tamper-proof narcotic delivery system |
| US20030008409A1 (en) * | 2001-07-03 | 2003-01-09 | Spearman Steven R. | Method and apparatus for determining sunlight exposure |
| CA2452874A1 (en) | 2001-07-06 | 2003-01-16 | Endo Pharmaceuticals, Inc. | Oral administration of 6-hydroxy-oxymorphone for use as an analgesic |
| US8329216B2 (en) | 2001-07-06 | 2012-12-11 | Endo Pharmaceuticals Inc. | Oxymorphone controlled release formulations |
| PL207748B1 (en) | 2001-07-06 | 2011-01-31 | Penwest Pharmaceuticals Company | Sustained release formulations of oxymorphone |
| JP2003020517A (en) | 2001-07-10 | 2003-01-24 | Calp Corp | Resin composition for compound fiber |
| PT1416842E (en) | 2001-07-18 | 2009-03-31 | Euro Celtique Sa | Pharmaceutical combinations of oxycodone and naloxone |
| US6883976B2 (en) | 2001-07-30 | 2005-04-26 | Seikoh Giken Co., Ltd. | Optical fiber ferrule assembly and optical module and optical connector using the same |
| US7332182B2 (en) | 2001-08-06 | 2008-02-19 | Purdue Pharma L.P. | Pharmaceutical formulation containing opioid agonist, opioid antagonist and irritant |
| CA2455420A1 (en) | 2001-08-06 | 2003-02-20 | Euro-Celtique, S.A. | Compositions and methods to prevent abuse of opioids |
| US7144587B2 (en) | 2001-08-06 | 2006-12-05 | Euro-Celtique S.A. | Pharmaceutical formulation containing opioid agonist, opioid antagonist and bittering agent |
| WO2003015531A2 (en) | 2001-08-06 | 2003-02-27 | Thomas Gruber | Pharmaceutical formulation containing dye |
| US7141250B2 (en) | 2001-08-06 | 2006-11-28 | Euro-Celtique S.A. | Pharmaceutical formulation containing bittering agent |
| US20030157168A1 (en) | 2001-08-06 | 2003-08-21 | Christopher Breder | Sequestered antagonist formulations |
| US20030068375A1 (en) * | 2001-08-06 | 2003-04-10 | Curtis Wright | Pharmaceutical formulation containing gelling agent |
| US7842307B2 (en) * | 2001-08-06 | 2010-11-30 | Purdue Pharma L.P. | Pharmaceutical formulation containing opioid agonist, opioid antagonist and gelling agent |
| US20030044458A1 (en) | 2001-08-06 | 2003-03-06 | Curtis Wright | Oral dosage form comprising a therapeutic agent and an adverse-effect agent |
| CA2456322A1 (en) | 2001-08-06 | 2003-02-20 | Euro-Celtique, S.A. | Compositions and methods to prevent abuse of opioids |
| US7157103B2 (en) | 2001-08-06 | 2007-01-02 | Euro-Celtique S.A. | Pharmaceutical formulation containing irritant |
| US20030049272A1 (en) | 2001-08-30 | 2003-03-13 | Yatindra Joshi | Pharmaceutical composition which produces irritation |
| US6691698B2 (en) | 2001-09-14 | 2004-02-17 | Fmc Technologies Inc. | Cooking oven having curved heat exchanger |
| US20030059467A1 (en) | 2001-09-14 | 2003-03-27 | Pawan Seth | Pharmaceutical composition comprising doxasozin |
| US20030059397A1 (en) | 2001-09-17 | 2003-03-27 | Lyn Hughes | Dosage forms |
| US20030068276A1 (en) * | 2001-09-17 | 2003-04-10 | Lyn Hughes | Dosage forms |
| US20030092724A1 (en) | 2001-09-18 | 2003-05-15 | Huaihung Kao | Combination sustained release-immediate release oral dosage forms with an opioid analgesic and a non-opioid analgesic |
| US20050019399A1 (en) * | 2001-09-21 | 2005-01-27 | Gina Fischer | Controlled release solid dispersions |
| US20040253310A1 (en) | 2001-09-21 | 2004-12-16 | Gina Fischer | Morphine polymer release system |
| EP1429735A2 (en) | 2001-09-26 | 2004-06-23 | Klaus-Jürgen Steffens | Method and device for producing granulates that comprise at least one pharmaceutical active substance |
| US20030091635A1 (en) | 2001-09-26 | 2003-05-15 | Baichwal Anand R. | Opioid formulations having reduced potential for abuse |
| JP2005508325A (en) | 2001-09-28 | 2005-03-31 | マクニール−ピーピーシー・インコーポレイテッド | Dosage form having an inner core and an outer shell |
| US6837696B2 (en) | 2001-09-28 | 2005-01-04 | Mcneil-Ppc, Inc. | Apparatus for manufacturing dosage forms |
| MXPA04003306A (en) | 2001-10-09 | 2004-07-23 | Procter & Gamble | Aqueous compositions for treating a surface. |
| US6592901B2 (en) | 2001-10-15 | 2003-07-15 | Hercules Incorporated | Highly compressible ethylcellulose for tableting |
| JP2003125706A (en) | 2001-10-23 | 2003-05-07 | Lion Corp | Mouth freshening preparation |
| PE20030527A1 (en) | 2001-10-24 | 2003-07-26 | Gruenenthal Chemie | DELAYED-RELEASE PHARMACEUTICAL FORMULATION CONTAINING 3- (3-DIMETHYLAMINO-1-ETHYL-2-METHYL-PROPYL) PHENOL OR A PHARMACEUTICALLY ACCEPTABLE SALT OF THE SAME AND ORAL TABLETS CONTAINING IT |
| CA2409552A1 (en) | 2001-10-25 | 2003-04-25 | Depomed, Inc. | Gastric retentive oral dosage form with restricted drug release in the lower gastrointestinal tract |
| US6723340B2 (en) * | 2001-10-25 | 2004-04-20 | Depomed, Inc. | Optimal polymer mixtures for gastric retentive tablets |
| US20030091630A1 (en) | 2001-10-25 | 2003-05-15 | Jenny Louie-Helm | Formulation of an erodible, gastric retentive oral dosage form using in vitro disintegration test data |
| US20030104052A1 (en) | 2001-10-25 | 2003-06-05 | Bret Berner | Gastric retentive oral dosage form with restricted drug release in the lower gastrointestinal tract |
| TWI312285B (en) * | 2001-10-25 | 2009-07-21 | Depomed Inc | Methods of treatment using a gastric retained gabapentin dosage |
| US20030152622A1 (en) | 2001-10-25 | 2003-08-14 | Jenny Louie-Helm | Formulation of an erodible, gastric retentive oral diuretic |
| US7300668B2 (en) | 2001-10-29 | 2007-11-27 | Massachusetts Institute Of Technology | System for manufacturing controlled release dosage forms, such as a zero-order release profile dosage form manufactured by three-dimensional printing |
| EP1450824A4 (en) | 2001-11-02 | 2005-09-28 | Elan Corp Plc | Pharmaceutical composition |
| US20040126428A1 (en) | 2001-11-02 | 2004-07-01 | Lyn Hughes | Pharmaceutical formulation including a resinate and an aversive agent |
| CA2484528A1 (en) | 2001-12-06 | 2003-06-19 | Michael P. Hite | Isoflavone composition for oral delivery |
| FR2833838B1 (en) | 2001-12-21 | 2005-09-16 | Ellipse Pharmaceuticals | METHOD FOR MANUFACTURING A TABLET INCLUDING A MORPHINIC ANALGESIC AND TABLET OBTAINED |
| AUPS044502A0 (en) | 2002-02-11 | 2002-03-07 | Commonwealth Scientific And Industrial Research Organisation | Novel catalysts and processes for their preparation |
| US20040033253A1 (en) | 2002-02-19 | 2004-02-19 | Ihor Shevchuk | Acyl opioid antagonists |
| US20030158265A1 (en) | 2002-02-20 | 2003-08-21 | Ramachandran Radhakrishnan | Orally administrable pharmaceutical formulation comprising pseudoephedrine hydrochloride and process for preparing the same |
| US20030190343A1 (en) | 2002-03-05 | 2003-10-09 | Pfizer Inc. | Palatable pharmaceutical compositions for companion animals |
| US6572889B1 (en) * | 2002-03-07 | 2003-06-03 | Noveon Ip Holdings Corp. | Controlled release solid dosage carbamazepine formulations |
| US6753009B2 (en) * | 2002-03-13 | 2004-06-22 | Mcneil-Ppc, Inc. | Soft tablet containing high molecular weight polyethylene oxide |
| SI2425824T1 (en) | 2002-04-05 | 2017-06-30 | Mundipharma Medical Cee Gmbh | Pharmaceutical preparation containing oxycodone and naloxone |
| DE10217232B4 (en) | 2002-04-18 | 2004-08-19 | Ticona Gmbh | Process for the production of filled granules from polyethylene of high or ultra-high molecular weight |
| US6960617B2 (en) | 2002-04-22 | 2005-11-01 | Purdue Research Foundation | Hydrogels having enhanced elasticity and mechanical strength properties |
| CN1665482A (en) | 2002-04-29 | 2005-09-07 | 阿尔扎公司 | Methods and dosage forms for controlled delivery of oxycodone |
| US20050106249A1 (en) | 2002-04-29 | 2005-05-19 | Stephen Hwang | Once-a-day, oral, controlled-release, oxycodone dosage forms |
| AU2003234395B2 (en) | 2002-05-13 | 2008-01-24 | Endo Pharmaceuticals Inc. | Abuse-resistant opioid solid dosage form |
| WO2003101384A2 (en) | 2002-05-31 | 2003-12-11 | Alza Corporation | Dosage forms and compositions for osmotic delivery of variable dosages of oxycodone |
| DE10250083A1 (en) | 2002-06-17 | 2003-12-24 | Gruenenthal Gmbh | Dosage form protected against abuse |
| US7776314B2 (en) | 2002-06-17 | 2010-08-17 | Grunenthal Gmbh | Abuse-proofed dosage system |
| CA2491572C (en) | 2002-07-05 | 2010-03-23 | Collegium Pharmaceutical, Inc. | Abuse-deterrent pharmaceutical compositions of opiods and other drugs |
| US20040011806A1 (en) | 2002-07-17 | 2004-01-22 | Luciano Packaging Technologies, Inc. | Tablet filler device with star wheel |
| US20070196481A1 (en) | 2002-07-25 | 2007-08-23 | Amidon Gregory E | Sustained-release tablet composition |
| US7388068B2 (en) | 2002-08-21 | 2008-06-17 | Clariant Produkte (Deutschland) Gmbh | Copolymers made of alkylene oxides and glycidyl ethers and use thereof as polymerizable emulsifiers |
| JP2006501234A (en) | 2002-08-21 | 2006-01-12 | フォークス ファーマシューティカルズ リミテッド | Use of water-soluble sugar aqueous solutions such as citric acid and lactitol as tableting solutions in tablet production |
| US20040052844A1 (en) * | 2002-09-16 | 2004-03-18 | Fang-Hsiung Hsiao | Time-controlled, sustained release, pharmaceutical composition containing water-soluble resins |
| ES2315530T3 (en) | 2002-09-17 | 2009-04-01 | Wyeth | GRANULATED FORMULATION OF A RAPAMYCIN ESTER CCI-779. |
| EP1539098B1 (en) | 2002-09-20 | 2011-08-10 | Fmc Corporation | Cosmetic composition containing microcrystalline cellulose |
| WO2004026308A1 (en) | 2002-09-21 | 2004-04-01 | Shuyi Zhang | Sustained release compound of acetamidophenol and tramadol |
| CA2499994C (en) | 2002-09-23 | 2012-07-10 | Verion, Inc. | Abuse-resistant pharmaceutical compositions |
| JP2004143071A (en) | 2002-10-23 | 2004-05-20 | Hosokawa Funtai Gijutsu Kenkyusho:Kk | Method for producing medicine-containing composite particle and medicine-containing composite particle |
| DE10250087A1 (en) | 2002-10-25 | 2004-05-06 | Grünenthal GmbH | Dosage form protected against abuse |
| US20050191244A1 (en) | 2002-10-25 | 2005-09-01 | Gruenenthal Gmbh | Abuse-resistant pharmaceutical dosage form |
| US20050186139A1 (en) * | 2002-10-25 | 2005-08-25 | Gruenenthal Gmbh | Abuse-proofed dosage form |
| DE10250084A1 (en) | 2002-10-25 | 2004-05-06 | Grünenthal GmbH | Dosage form protected against abuse |
| DE10250088A1 (en) | 2002-10-25 | 2004-05-06 | Grünenthal GmbH | Dosage form protected against abuse |
| PT1594460E (en) | 2002-10-25 | 2008-06-27 | Labopharm Inc | Sustained-release tramadol formulations with 24-hour efficacy |
| DE10252667A1 (en) * | 2002-11-11 | 2004-05-27 | Grünenthal GmbH | New spiro-((cyclohexane)-tetrahydropyrano-(3,4-b)-indole) derivatives, are ORL1 receptor ligands useful e.g. for treating anxiety, depression, epilepsy, senile dementia, withdrawal symptoms or especially pain |
| US20040091528A1 (en) | 2002-11-12 | 2004-05-13 | Yamanouchi Pharma Technologies, Inc. | Soluble drug extended release system |
| US7018658B2 (en) | 2002-11-14 | 2006-03-28 | Synthon Bv | Pharmaceutical pellets comprising tamsulosin |
| US20040121003A1 (en) | 2002-12-19 | 2004-06-24 | Acusphere, Inc. | Methods for making pharmaceutical formulations comprising deagglomerated microparticles |
| US20040185097A1 (en) | 2003-01-31 | 2004-09-23 | Glenmark Pharmaceuticals Ltd. | Controlled release modifying complex and pharmaceutical compositions thereof |
| US7442387B2 (en) | 2003-03-06 | 2008-10-28 | Astellas Pharma Inc. | Pharmaceutical composition for controlled release of active substances and manufacturing method thereof |
| DE602004024963D1 (en) * | 2003-03-13 | 2010-02-25 | Controlled Chemicals Inc | OXYCODON CONJUGATES WITH LOWER ABUSE POTENTIAL AND EXTENDED ACTIVITY |
| CA2520312C (en) | 2003-03-26 | 2013-06-18 | Egalet A/S | Matrix compositions for controlled delivery of drug substances |
| ATE495732T1 (en) | 2003-03-26 | 2011-02-15 | Egalet As | CONTROLLED RELEASE MORPHINE SYSTEM |
| CN1767831B (en) * | 2003-04-08 | 2014-12-10 | 普罗热尼奇制药公司 | Pharmaceutical formulations containing methylnaltrexone |
| TWI347201B (en) | 2003-04-21 | 2011-08-21 | Euro Celtique Sa | Pharmaceutical products,uses thereof and methods for preparing the same |
| CA2519556C (en) | 2003-04-21 | 2011-01-18 | Benjamin Oshlack | Tamper resistant dosage form comprising co-extruded, adverse agent particles and process of making same |
| CL2004000927A1 (en) | 2003-04-30 | 2005-01-28 | Purdue Pharma Lp | TRANSDERMAL DOSAGE FORM THAT INCLUDES AN ACTIVE AGENT, A NEXT SURFACE AND A DISTAL SURFACE. |
| US8906413B2 (en) | 2003-05-12 | 2014-12-09 | Supernus Pharmaceuticals, Inc. | Drug formulations having reduced abuse potential |
| CN1473562A (en) | 2003-06-27 | 2004-02-11 | 辉 刘 | Mouth cavity quick dissolving quick disintegrating freeze-dried tablet and its preparing method |
| US20050015730A1 (en) | 2003-07-14 | 2005-01-20 | Srimanth Gunturi | Systems, methods and computer program products for identifying tab order sequence of graphically represented elements |
| RU2339365C2 (en) | 2003-08-06 | 2008-11-27 | Грюненталь Гмбх | Drug dosage form, protected from unintended application |
| US20070048228A1 (en) * | 2003-08-06 | 2007-03-01 | Elisabeth Arkenau-Maric | Abuse-proofed dosage form |
| US8075872B2 (en) * | 2003-08-06 | 2011-12-13 | Gruenenthal Gmbh | Abuse-proofed dosage form |
| DE10361596A1 (en) | 2003-12-24 | 2005-09-29 | Grünenthal GmbH | Process for producing an anti-abuse dosage form |
| DE102005005446A1 (en) | 2005-02-04 | 2006-08-10 | Grünenthal GmbH | Break-resistant dosage forms with sustained release |
| CA2534925A1 (en) | 2003-08-06 | 2005-02-24 | Gruenenthal Gmbh | Dosage form that is safeguarded from abuse |
| DE102004032051A1 (en) * | 2004-07-01 | 2006-01-19 | Grünenthal GmbH | Process for the preparation of a secured against misuse, solid dosage form |
| DE102004020220A1 (en) | 2004-04-22 | 2005-11-10 | Grünenthal GmbH | Process for the preparation of a secured against misuse, solid dosage form |
| DE10336400A1 (en) | 2003-08-06 | 2005-03-24 | Grünenthal GmbH | Anti-abuse dosage form |
| US20050063214A1 (en) | 2003-09-22 | 2005-03-24 | Daisaburo Takashima | Semiconductor integrated circuit device |
| DE602004026604D1 (en) | 2003-09-25 | 2010-05-27 | Euro Celtique Sa | PHARMACEUTICAL COMBINATIONS OF HYDROCODON AND NALTREXONE |
| BRPI0414941A (en) | 2003-09-30 | 2006-11-07 | Alza Corp | osmotically driven active agent dispensing device providing an upward release profile |
| US20060172006A1 (en) | 2003-10-10 | 2006-08-03 | Vincent Lenaerts | Sustained-release tramadol formulations with 24-hour clinical efficacy |
| US20060009478A1 (en) * | 2003-10-15 | 2006-01-12 | Nadav Friedmann | Methods for the treatment of back pain |
| EP1677798A2 (en) | 2003-10-29 | 2006-07-12 | Alza Corporation | Once-a-day, oral, controlled-release, oxycodone dosage forms |
| US7201920B2 (en) | 2003-11-26 | 2007-04-10 | Acura Pharmaceuticals, Inc. | Methods and compositions for deterring abuse of opioid containing dosage forms |
| JP2007513147A (en) | 2003-12-04 | 2007-05-24 | ファイザー・プロダクツ・インク | Spray congealing process for producing a multiparticulate crystalline pharmaceutical composition, preferably containing poloxamer and glyceride, using an extruder |
| US20070269505A1 (en) | 2003-12-09 | 2007-11-22 | Flath Robert P | Tamper Resistant Co-Extruded Dosage Form Containing An Active Agent And An Adverse Agent And Process Of Making Same |
| WO2005060942A1 (en) | 2003-12-19 | 2005-07-07 | Aurobindo Pharma Ltd | Extended release pharmaceutical composition of metformin |
| DE10360792A1 (en) | 2003-12-23 | 2005-07-28 | Grünenthal GmbH | Spirocyclic cyclohexane derivatives |
| CA2551815A1 (en) | 2003-12-29 | 2005-07-21 | Alza Corporation | Novel drug compositions and dosage forms |
| WO2005079752A2 (en) | 2004-02-11 | 2005-09-01 | Rubicon Research Private Limited | Controlled release pharmaceutical compositions with improved bioavailability |
| GB0403098D0 (en) | 2004-02-12 | 2004-03-17 | Euro Celtique Sa | Extrusion |
| TWI350762B (en) | 2004-02-12 | 2011-10-21 | Euro Celtique Sa | Particulates |
| GB0403100D0 (en) | 2004-02-12 | 2004-03-17 | Euro Celtique Sa | Particulates |
| LT2351555T (en) | 2004-02-23 | 2016-12-27 | Euro-Celtique S.A. | Abuse resistance opioid transdermal delivery device |
| TW201509943A (en) | 2004-03-30 | 2015-03-16 | Euro Celtique Sa | Oxycodone hydrochloride composition, pharmaceutical dosage form, sustained release oral dosage form and pharmaceutically acceptable package having less than 25 PPM 14-hydroxycodeinone |
| US20050220877A1 (en) | 2004-03-31 | 2005-10-06 | Patel Ashish A | Bilayer tablet comprising an antihistamine and a decongestant |
| DE102004019916A1 (en) | 2004-04-21 | 2005-11-17 | Grünenthal GmbH | Anti-abuse drug-containing patch |
| WO2005102286A1 (en) | 2004-04-22 | 2005-11-03 | Grünenthal GmbH | Method for the production of an abuse-proof, solid form of administration |
| WO2005105036A1 (en) | 2004-04-28 | 2005-11-10 | Natco Pharma Limited | Controlled release mucoadhesive matrix formulation containing tolterodine and a process for its preparation |
| US20050271594A1 (en) | 2004-06-04 | 2005-12-08 | Groenewoud Pieter J | Abuse resistent pharmaceutical composition |
| TWI547431B (en) * | 2004-06-09 | 2016-09-01 | 史密斯克萊美占公司 | Apparatus and method for pharmaceutical production |
| PL1612203T3 (en) | 2004-06-28 | 2007-12-31 | Gruenenthal Gmbh | Crystalline forms of (-)-(1R,2R)-3-(3-dimethylamino-1-ethyl-2-methylpropyl)-phenol hydrochloride |
| ITMI20041317A1 (en) | 2004-06-30 | 2004-09-30 | Ibsa Inst Biochimique Sa | PHARMACEUTICAL FORMULATIONS FOR THE SAFE ADMINISTRATION OF DRUGS USED IN THE TREATMENT OF DRUG ADDICTION AND PROCEDURE FOR THEIR OBTAINING |
| AR049839A1 (en) | 2004-07-01 | 2006-09-06 | Gruenenthal Gmbh | PROCEDURE FOR THE PRODUCTION OF A SOLID PHARMACEUTICAL FORM, PROTECTED AGAINST ABUSE |
| PL1765303T5 (en) | 2004-07-01 | 2023-05-22 | Grünenthal GmbH | Oral dosage form safeguarded against abuse |
| DE102004032103A1 (en) * | 2004-07-01 | 2006-01-19 | Grünenthal GmbH | Anti-abuse, oral dosage form |
| DE102004032049A1 (en) | 2004-07-01 | 2006-01-19 | Grünenthal GmbH | Anti-abuse, oral dosage form |
| AR053304A1 (en) | 2004-07-01 | 2007-05-02 | Gruenenthal Gmbh | PROTECTED ORAL PHARMACEUTICAL FORMS AGAINST ABUSE WITH CONTROLLED RELEASE OF (1R, 2R) -3- (3 DIMETHYLAMIN-1-ETIL-2METIL-PROPIL) PHENOL AND PROCEDURE FOR PRODUCTION. |
| KR20060007225A (en) * | 2004-07-19 | 2006-01-24 | 삼성전자주식회사 | Auto-stabilization method in control of driving image pickup device and reading memory and apparatus thereof |
| US7947259B2 (en) | 2004-07-27 | 2011-05-24 | Conopco, Inc. | Hair care compositions |
| US20060021410A1 (en) * | 2004-07-30 | 2006-02-02 | Sonats-Societe Des Nouvelles Applications Des Techniques De Surfaces | Shot, devices, and installations for ultrasonic peening, and parts treated thereby |
| US20070077297A1 (en) | 2004-09-30 | 2007-04-05 | Scolr Pharma, Inc. | Modified release ibuprofen dosage form |
| US20060068009A1 (en) | 2004-09-30 | 2006-03-30 | Scolr Pharma, Inc. | Modified release ibuprofen dosage form |
| US7426948B2 (en) | 2004-10-08 | 2008-09-23 | Phibrowood, Llc | Milled submicron organic biocides with narrow particle size distribution, and uses thereof |
| US20080152595A1 (en) | 2004-11-24 | 2008-06-26 | Acura Pharmaceuticals, Inc. | Methods and compositions for deterring abuse of orally administered pharmaceutical products |
| US20060177380A1 (en) | 2004-11-24 | 2006-08-10 | Acura Pharmaceuticals, Inc. | Methods and compositions for deterring abuse of orally administered pharmaceutical products |
| US20070231268A1 (en) | 2004-11-24 | 2007-10-04 | Acura Pharmaceuticals, Inc. | Methods and compositions for deterring abuse of orally administered pharmaceutical products |
| PT1849470T (en) | 2005-01-26 | 2017-09-22 | Taiho Pharmaceutical Co Ltd | Anticancer drug containing alpha, alpha, alpha-trifluorothymidine and thymidine phosphorylase inhibitor |
| MX2007009162A (en) | 2005-01-28 | 2007-10-23 | Euro Celtique Sa | Alcohol resistant dosage forms. |
| DE102005005449A1 (en) | 2005-02-04 | 2006-08-10 | Grünenthal GmbH | Process for producing an anti-abuse dosage form |
| FR2889810A1 (en) | 2005-05-24 | 2007-02-23 | Flamel Technologies Sa | ORAL MEDICINAL FORM, MICROPARTICULAR, ANTI-MEASUREMENT |
| EP1853249A2 (en) * | 2005-02-10 | 2007-11-14 | LifeCycle Pharma A/S | A stable pharmaceutical composition comprising a fixed dose combination of fenofibrate and an hmg-coa reductase inhibitor |
| US20060194759A1 (en) | 2005-02-25 | 2006-08-31 | Eidelson Stewart G | Topical compositions and methods for treating pain and inflammation |
| EP1695700A1 (en) | 2005-02-28 | 2006-08-30 | Euro-Celtique S.A. | Dosage form containing oxycodone and naloxone |
| KR100941761B1 (en) * | 2005-03-04 | 2010-02-11 | 유로-셀띠끄 소시에떼 아노님 | Method of reducing alpha, beta unsaturated ketones in opioid compositions |
| US20060204575A1 (en) | 2005-03-11 | 2006-09-14 | Hengsheng Feng | Amphetamine formulations |
| US7732427B2 (en) | 2005-03-31 | 2010-06-08 | University Of Delaware | Multifunctional and biologically active matrices from multicomponent polymeric solutions |
| CN101227892B (en) | 2005-04-08 | 2013-06-05 | 舌交付有限公司 | Buccal delivery system |
| RU2405539C2 (en) | 2005-05-10 | 2010-12-10 | Новартис Аг | Method of obtaining compositions by extrusion of resistant to pressing pharmaceutical substances |
| AU2006254554B2 (en) | 2005-06-03 | 2011-11-24 | Egalet Ltd | A solid pharmaceutical composition with a first fraction of a dispersion medium and a second fraction of a matrix, the latter being at least partially first exposed to gastrointestinal fluids |
| WO2007005716A2 (en) | 2005-06-30 | 2007-01-11 | Cinergen, Llc | Methods of treatment and compositions for use thereof |
| BRPI0612802A2 (en) | 2005-07-07 | 2010-11-30 | Farnam Co Inc | sustained release pharmaceutical compositions for extremely water soluble drugs |
| DE102005032806A1 (en) | 2005-07-12 | 2007-01-18 | Röhm Gmbh | Use of a partially neutralized, anionic (meth) acrylate copolymer as a coating for the preparation of a dosage form with a release of active ingredient at reduced pH values |
| US8858993B2 (en) | 2005-07-25 | 2014-10-14 | Metrics, Inc. | Coated tablet with zero-order or near zero-order release kinetics |
| US20070184117A1 (en) | 2005-08-03 | 2007-08-09 | Stephen Gregory | Tocopheryl polyethylene glycol succinate powder and process for preparing same |
| US20070048373A1 (en) | 2005-08-30 | 2007-03-01 | Cima Labs Inc. | Dried milled granulate and methods |
| EP1950219B1 (en) | 2005-10-14 | 2011-06-22 | The Kitasato Institute | Novel dihydropseudoerythromycin derivatives |
| US20070092573A1 (en) | 2005-10-24 | 2007-04-26 | Laxminarayan Joshi | Stabilized extended release pharmaceutical compositions comprising a beta-adrenoreceptor antagonist |
| PL116330U1 (en) | 2005-10-31 | 2007-04-02 | Alza Corp | Method for the reduction of alcohol provoked rapid increase in the released dose of the orally administered opioide with prolonged liberation |
| US8329744B2 (en) | 2005-11-02 | 2012-12-11 | Relmada Therapeutics, Inc. | Methods of preventing the serotonin syndrome and compositions for use thereof |
| US9125833B2 (en) | 2005-11-02 | 2015-09-08 | Relmada Therapeutics, Inc. | Multimodal abuse resistant and extended release opioid formulations |
| US8652529B2 (en) * | 2005-11-10 | 2014-02-18 | Flamel Technologies | Anti-misuse microparticulate oral pharmaceutical form |
| FR2892937B1 (en) | 2005-11-10 | 2013-04-05 | Flamel Tech Sa | MICROPARTICULAR ORAL PHARMACEUTICAL FORM ANTI-MEASURING |
| DE102005058569B4 (en) | 2005-12-08 | 2010-07-15 | Lts Lohmann Therapie-Systeme Ag | Foam wafer with polyvinyl alcohol-polyethylene glycol graft copolymer |
| JP2009523833A (en) | 2006-01-21 | 2009-06-25 | アボット ゲーエムベーハー ウント カンパニー カーゲー | Formulations and methods for drug delivery |
| US20090317355A1 (en) | 2006-01-21 | 2009-12-24 | Abbott Gmbh & Co. Kg, | Abuse resistant melt extruded formulation having reduced alcohol interaction |
| US20090022798A1 (en) * | 2007-07-20 | 2009-01-22 | Abbott Gmbh & Co. Kg | Formulations of nonopioid and confined opioid analgesics |
| US20100172989A1 (en) | 2006-01-21 | 2010-07-08 | Abbott Laboratories | Abuse resistant melt extruded formulation having reduced alcohol interaction |
| EP1813276A1 (en) | 2006-01-27 | 2007-08-01 | Euro-Celtique S.A. | Tamper resistant dosage forms |
| FR2897267A1 (en) | 2006-02-16 | 2007-08-17 | Flamel Technologies Sa | MULTIMICROPARTICULAR PHARMACEUTICAL FORMS FOR PER OS ADMINISTRATION |
| ZA200807571B (en) * | 2006-03-01 | 2009-08-26 | Ethypharm Sa | Crush-resistant tablets intended to prevent accidental misuse and unlawful diversion |
| AU2007224221B2 (en) | 2006-03-02 | 2013-02-14 | SpecGx LLC | Processes for preparing morphinan-6-one products with low levels of alpha, beta-unsaturated ketone compounds |
| EP2086515A2 (en) | 2006-03-02 | 2009-08-12 | Vaunnex, Inc. | Rate-controlled bioadhesive oral dosage formulations |
| US20070224637A1 (en) | 2006-03-24 | 2007-09-27 | Mcauliffe Joseph C | Oxidative protection of lipid layer biosensors |
| AU2007230730B2 (en) | 2006-03-24 | 2013-03-28 | Auxilium International Holdings, Inc. | Stabilized compositions containing alkaline labile drugs |
| JP5336351B2 (en) * | 2006-03-24 | 2013-11-06 | オクシリウム インターナショナル ホールディングス,インコーポレイティド | Method for preparing hot melt extruded laminate |
| US10960077B2 (en) | 2006-05-12 | 2021-03-30 | Intellipharmaceutics Corp. | Abuse and alcohol resistant drug composition |
| US9023400B2 (en) | 2006-05-24 | 2015-05-05 | Flamel Technologies | Prolonged-release multimicroparticulate oral pharmaceutical form |
| WO2007138466A2 (en) | 2006-06-01 | 2007-12-06 | Wockhardt Ltd | Pharmaceutical compositions comprising meloxicam and tramadol combination |
| US20070292508A1 (en) | 2006-06-05 | 2007-12-20 | Balchem Corporation | Orally disintegrating dosage forms |
| US20080069891A1 (en) | 2006-09-15 | 2008-03-20 | Cima Labs, Inc. | Abuse resistant drug formulation |
| CN101091721A (en) | 2006-06-22 | 2007-12-26 | 孙明 | Method for preparing new type asshide |
| EP2043613A1 (en) | 2006-07-14 | 2009-04-08 | Fmc Corporation | Solid form |
| JP4029109B1 (en) | 2006-07-18 | 2008-01-09 | タマ生化学株式会社 | Complex powder of vitamin E and proline and method for producing the same |
| WO2008011596A2 (en) * | 2006-07-21 | 2008-01-24 | Lab International Srl | Hydrophilic abuse deterrent delivery system |
| SA07280459B1 (en) | 2006-08-25 | 2011-07-20 | بيورديو فارما إل. بي. | Tamper Resistant Oral Pharmaceutical Dosage Forms Comprising an Opioid Analgesic |
| US8445018B2 (en) | 2006-09-15 | 2013-05-21 | Cima Labs Inc. | Abuse resistant drug formulation |
| US8187636B2 (en) | 2006-09-25 | 2012-05-29 | Atlantic Pharmaceuticals, Inc. | Dosage forms for tamper prone therapeutic agents |
| KR101400824B1 (en) * | 2006-09-25 | 2014-05-29 | 후지필름 가부시키가이샤 | Resist composition, resin for use in the resist composition, compound for use in the synthesis of the resin, and pattern-forming method usign the resist composition |
| MX2009003771A (en) | 2006-10-10 | 2009-07-22 | Penwest Pharmaceuticals Co | Robust sustained release formulations. |
| US20080085304A1 (en) | 2006-10-10 | 2008-04-10 | Penwest Pharmaceuticals Co. | Robust sustained release formulations |
| GB0624880D0 (en) | 2006-12-14 | 2007-01-24 | Johnson Matthey Plc | Improved method for making analgesics |
| WO2008079404A2 (en) | 2006-12-22 | 2008-07-03 | Combinatorx, Incorporated | Pharmaceutical compositions for treatment of parkinson's disease and related disorders |
| DE102006062120A1 (en) * | 2006-12-22 | 2008-06-26 | Grünenthal GmbH | Pharmaceutical composition for acne treatment |
| EP2104493A2 (en) | 2007-01-16 | 2009-09-30 | Egalet A/S | Use of i) a polyglycol and n) an active drug substance for the preparation of a pharmaceutical composition for i) mitigating the risk of alcohol induced dose dumping and/or ii) reducing the risk of drug abuse |
| WO2008094877A2 (en) | 2007-01-30 | 2008-08-07 | Drugtech Corporation | Compositions for oral delivery of pharmaceuticals |
| CN100579525C (en) | 2007-02-02 | 2010-01-13 | 东南大学 | Sustained release preparation of licardipine hydrochloride and its preparing process |
| BRPI0807157A2 (en) | 2007-02-08 | 2014-04-29 | Kempharm Inc | POLY HYDROPHYAL PROPHARMACIES OF AMPHTAMINE AND OTHER STIMULANTS AND PROCESSES FOR THE MANUFACTURE AND USE OF THE SAME |
| CN101057849A (en) | 2007-02-27 | 2007-10-24 | 齐齐哈尔医学院 | Slow-releasing preparation containing metformin hydrochloride and glipizide and its preparation method |
| ATE476176T1 (en) | 2007-03-02 | 2010-08-15 | Farnam Co Inc | SUSTAINED-RELEASE TABLETS CONTAINING WAX-LIKE MATERIAL |
| DE102007011485A1 (en) * | 2007-03-07 | 2008-09-11 | Grünenthal GmbH | Dosage form with more difficult abuse |
| EP1980245A1 (en) | 2007-04-11 | 2008-10-15 | Cephalon France | Bilayer lyophilized pharmaceutical compositions and methods of making and using same |
| US20080260836A1 (en) | 2007-04-18 | 2008-10-23 | Thomas James Boyd | Films Comprising a Plurality of Polymers |
| CA2685118C (en) | 2007-04-26 | 2016-11-01 | Sigmoid Pharma Limited | Manufacture of multiple minicapsules |
| US20110020408A1 (en) | 2007-05-17 | 2011-01-27 | Ranbaxy Laboratories Limited | multilayered modified release formulation comprising amoxicillin and clavulanate |
| US8202542B1 (en) | 2007-05-31 | 2012-06-19 | Tris Pharma | Abuse resistant opioid drug-ion exchange resin complexes having hybrid coatings |
| EP2155167A2 (en) | 2007-06-04 | 2010-02-24 | Egalet A/S | Controlled release pharmaceutical compositions for prolonged effect |
| US20100035886A1 (en) | 2007-06-21 | 2010-02-11 | Veroscience, Llc | Parenteral formulations of dopamine agonists |
| EP2170051A1 (en) | 2007-07-01 | 2010-04-07 | Joseph Peter Habboushe | Combination tablet with chewable outer layer |
| CN101917977B (en) | 2007-07-20 | 2013-05-29 | 艾博特股份有限两合公司 | Formulations of nonopioid and confined opioid analgesics |
| WO2009034541A2 (en) | 2007-09-11 | 2009-03-19 | Ranbaxy Laboratories Limited | Controlled release pharmaceutical dosage forms of trimetazidine |
| DK2200593T5 (en) | 2007-09-13 | 2016-12-12 | Cima Labs Inc | Hog-resistant pharmaceutical formulation |
| WO2009051819A1 (en) | 2007-10-17 | 2009-04-23 | Axxia Pharmaceuticals, Llc | Polymeric drug delivery systems and thermoplastic extrusion processes for producing such systems |
| EP3170494A3 (en) | 2007-11-23 | 2017-09-06 | Grünenthal GmbH | Tapentadol compositions |
| WO2009088414A2 (en) | 2007-12-06 | 2009-07-16 | Durect Corporation | Oral pharmaceutical dosage forms |
| WO2009074609A1 (en) | 2007-12-12 | 2009-06-18 | Basf Se | Salts of active ingredients with polymeric counter-ions |
| AU2008338207A1 (en) | 2007-12-17 | 2009-06-25 | Labopharm (Barbados) Limited | Misuse preventative, controlled release formulation |
| US8383152B2 (en) | 2008-01-25 | 2013-02-26 | Gruenenthal Gmbh | Pharmaceutical dosage form |
| KR100970665B1 (en) | 2008-02-04 | 2010-07-15 | 삼일제약주식회사 | Sustained release tablet containing alfuzosin or its salt |
| BRPI0901282A2 (en) | 2008-02-14 | 2009-11-17 | Ethicon Endo Surgery Inc | surgical cutting and fixation instrument with rf electrodes |
| AU2009220779A1 (en) | 2008-03-05 | 2009-09-11 | Panacea Biotec Limited | Modified release pharmaceutical compositions comprising mycophenolate and processes thereof |
| US8372432B2 (en) * | 2008-03-11 | 2013-02-12 | Depomed, Inc. | Gastric retentive extended-release dosage forms comprising combinations of a non-opioid analgesic and an opioid analgesic |
| EP2100598A1 (en) * | 2008-03-13 | 2009-09-16 | Laboratorios Almirall, S.A. | Inhalation composition containing aclidinium for treatment of asthma and chronic obstructive pulmonary disease |
| TWI519322B (en) | 2008-04-15 | 2016-02-01 | 愛戴爾製藥股份有限公司 | Compositions comprising weakly basic drugs and controlled-release dosage forms |
| HUE030803T2 (en) | 2008-05-09 | 2017-06-28 | Gruenenthal Gmbh | Process for the preparation of an intermediate powder formulation and a final solid dosage form under usage of a spray congealing step |
| JP2011526928A (en) * | 2008-07-03 | 2011-10-20 | ノバルティス アーゲー | Melt granulation method |
| MX2011001864A (en) | 2008-08-20 | 2011-06-20 | Univ Texas | Hot-melt extrusion of modified release multi-particulates. |
| FR2936709B1 (en) | 2008-10-02 | 2012-05-11 | Ethypharm Sa | ALCOHOL-RESISTANT TABLETS. |
| US20100099696A1 (en) * | 2008-10-16 | 2010-04-22 | Anthony Edward Soscia | Tamper resistant oral dosage forms containing an embolizing agent |
| CA2741751C (en) * | 2008-10-27 | 2017-05-09 | Alza Corporation | Extended release oral acetaminophen/tramadol dosage form |
| WO2010057036A2 (en) | 2008-11-14 | 2010-05-20 | Portola Pharmaceuticals, Inc. | Solid composition for controlled release of ionizable active agents with poor aqueous solubility at low ph and methods of use thereof |
| ES2414856T3 (en) | 2008-12-12 | 2013-07-23 | Paladin Labs Inc. | Narcotic drug formulations with decreased addiction potential |
| ES2509497T3 (en) | 2008-12-16 | 2014-10-17 | Paladin Labs Inc. | Controlled release formulation to prevent misuse |
| WO2010083843A1 (en) | 2009-01-26 | 2010-07-29 | Egalet A/S | Controlled release formulations with continuous efficacy |
| WO2010088911A1 (en) | 2009-02-06 | 2010-08-12 | Egalet A/S | Pharmaceutical compositions resistant to abuse |
| US9730899B2 (en) | 2009-03-18 | 2017-08-15 | Evonik Roehm Gmbh | Controlled release pharmaceutical composition with resistance against the influence of ethanol employing a coating comprising neutral vinyl polymers and excipients |
| EP2246063A1 (en) | 2009-04-29 | 2010-11-03 | Ipsen Pharma S.A.S. | Sustained release formulations comprising GnRH analogues |
| GB0909680D0 (en) | 2009-06-05 | 2009-07-22 | Euro Celtique Sa | Dosage form |
| NZ603579A (en) | 2009-06-24 | 2014-02-28 | Egalet Ltd | Controlled release formulations |
| WO2011008298A2 (en) | 2009-07-16 | 2011-01-20 | Nectid, Inc. | Novel axomadol dosage forms |
| RU2555531C2 (en) * | 2009-07-22 | 2015-07-10 | Грюненталь Гмбх | Misuse protected dosage form for oxidation sensitive opioids |
| KR101738369B1 (en) * | 2009-07-22 | 2017-05-22 | 그뤼넨탈 게엠베하 | Hot-melt extruded controlled release dosage form |
| EP3064064A1 (en) | 2009-09-30 | 2016-09-07 | Acura Pharmaceuticals, Inc. | Methods and compositions for deterring abuse |
| JP5529884B2 (en) | 2009-11-13 | 2014-06-25 | 森六ケミカルズ株式会社 | Method for producing fine powder and fine powder produced by the same method |
| EP2506838A1 (en) * | 2009-12-01 | 2012-10-10 | Noven Pharmaceuticals, INC. | Transdermal testosterone device and delivery |
| US9579285B2 (en) | 2010-02-03 | 2017-02-28 | Gruenenthal Gmbh | Preparation of a powdery pharmaceutical composition by means of an extruder |
| GB201003731D0 (en) | 2010-03-05 | 2010-04-21 | Univ Strathclyde | Immediate/delayed drug delivery |
| EA029077B1 (en) | 2010-03-09 | 2018-02-28 | Алкермес Фарма Айэленд Лимитед | Alcohol resistant pharmaceutical composition |
| CA2795158C (en) | 2010-04-02 | 2019-10-22 | Alltranz Inc. | Abuse-deterrent transdermal formulations of opiate agonists and agonist-antagonists |
| US9884022B2 (en) | 2010-04-07 | 2018-02-06 | Lupin Limited | Controlled release pharmaceutical compositions of tapentadol |
| GB201006200D0 (en) | 2010-04-14 | 2010-06-02 | Ayanda As | Composition |
| US10463633B2 (en) | 2010-04-23 | 2019-11-05 | Kempharm, Inc. | Therapeutic formulation for reduced drug side effects |
| US20130059010A1 (en) | 2010-05-14 | 2013-03-07 | Ethypharm | Alcohol-resistant oral pharmaceutical form |
| FR2960775A1 (en) | 2010-06-07 | 2011-12-09 | Ethypharm Sa | MICROGRANULES RESISTANT TO MISMATCH |
| AU2011297954B2 (en) | 2010-09-02 | 2014-05-15 | Grunenthal Gmbh | Tamper resistant dosage form comprising an anionic polymer |
| EP2611426B1 (en) | 2010-09-02 | 2014-06-25 | Grünenthal GmbH | Tamper resistant dosage form comprising inorganic salt |
| AR082862A1 (en) * | 2010-09-02 | 2013-01-16 | Gruenenthal Gmbh | ALTERATION RESISTANT DOSAGE FORM INCLUDING AN ANIONIC POLYMER |
| EP2635258A1 (en) | 2010-11-04 | 2013-09-11 | AbbVie Inc. | Drug formulations |
| US20120231083A1 (en) | 2010-11-18 | 2012-09-13 | The Board Of Trustees Of The University Of Illinois | Sustained release cannabinoid medicaments |
| GB201020895D0 (en) | 2010-12-09 | 2011-01-26 | Euro Celtique Sa | Dosage form |
| CN103327969A (en) | 2010-12-23 | 2013-09-25 | 普渡制药公司 | Tamper resistant solid oral dosage forms |
| MX2013009492A (en) | 2011-02-17 | 2014-07-30 | Qrxpharma Ltd | Technology for preventing abuse of solid dosage forms. |
| CN107308108A (en) | 2011-03-04 | 2017-11-03 | 格吕伦塔尔有限公司 | For the tapentadol hydrochloride aqueous medicament preparations orally given |
| SI2701693T1 (en) | 2011-04-29 | 2017-11-30 | Gruenenthal Gmbh | Tapentadol for preventing and treating depression and anxiety |
| US8858963B1 (en) | 2011-05-17 | 2014-10-14 | Mallinckrodt Llc | Tamper resistant composition comprising hydrocodone and acetaminophen for rapid onset and extended duration of analgesia |
| CA2837077A1 (en) | 2011-06-01 | 2012-12-06 | Fmc Corporation | Controlled release solid dose forms |
| EP2726065A4 (en) | 2011-06-30 | 2014-11-26 | Neos Therapeutics Lp | Abuse resistant drug forms |
| AR087359A1 (en) | 2011-07-29 | 2014-03-19 | Gruenenthal Gmbh | TEST ALTERATION TABLET PROVIDING IMMEDIATE RELEASE OF THE PHARMACO |
| EA201400172A1 (en) * | 2011-07-29 | 2014-06-30 | Грюненталь Гмбх | SUSTAINABLE TO DESTRUCTION TABLET THAT PROVIDES IMMEDIATE RELEASE OF MEDICINES |
| CA2844827A1 (en) | 2011-08-16 | 2013-02-21 | Merck Sharp & Dohme Corp. | Use of inorganic matrix and organic polymer combinations for preparing stable amorphous dispersions |
| FR2979242A1 (en) | 2011-08-29 | 2013-03-01 | Sanofi Sa | COMPRESSES AGAINST ABUSIVE USE, BASED ON PARACETAMOL AND OXYCODONE |
| KR20140075704A (en) | 2011-10-06 | 2014-06-19 | 그뤼넨탈 게엠베하 | Tamper-resistant oral pharmaceutical dosage form comprising opioid agonist and opioid antagonist |
| EA201400590A1 (en) | 2011-11-17 | 2014-11-28 | Грюненталь Гмбх | Resistance to fracture an oral pharmaceutical dosage form comprising a pharmacologically active ingredient opioid antagonist and / or a means, is disgusting, polyalkylene oxide and anionic polymers |
| TW201336529A (en) | 2011-12-09 | 2013-09-16 | Purdue Pharma Lp | Pharmaceutical dosage forms comprising poly( ε -caprolactone) and polyethylene oxide |
| JP2013155124A (en) | 2012-01-30 | 2013-08-15 | Moriroku Chemicals Co Ltd | Bulk powder of medicine and method of producing the same |
| WO2013127830A1 (en) | 2012-02-28 | 2013-09-06 | Grünenthal GmbH | Tamper-resistant pharmaceutical dosage form comprising nonionic surfactant |
| EP2819656A1 (en) | 2012-02-28 | 2015-01-07 | Grünenthal GmbH | Tamper-resistant dosage form comprising pharmacologically active compound and anionic polymer |
| WO2013128276A2 (en) | 2012-03-02 | 2013-09-06 | Rhodes Pharmaceuticals L.P. | Tamper resistant immediate release formulations |
| MX362357B (en) | 2012-04-18 | 2019-01-14 | Gruenenthal Gmbh | Tamper resistant and dose-dumping resistant pharmaceutical dosage form. |
| JP2015516406A (en) | 2012-05-11 | 2015-06-11 | グリュネンタール・ゲゼルシャフト・ミト・ベシュレンクテル・ハフツング | Thermoformed tamper-resistant pharmaceutical dosage forms containing zinc |
| US10064945B2 (en) | 2012-05-11 | 2018-09-04 | Gruenenthal Gmbh | Thermoformed, tamper-resistant pharmaceutical dosage form containing zinc |
| WO2014022541A1 (en) | 2012-08-01 | 2014-02-06 | Acura Pharmaceuticals, Inc. | Stabilization of one-pot methamphetamine synthesis systems |
| CN104507460A (en) | 2012-08-27 | 2015-04-08 | 赢创工业集团股份有限公司 | Gastric resistant pharmaceutical or nutraceutical composition with resistance against the influence of ethanol |
| JP5775223B2 (en) | 2012-09-05 | 2015-09-09 | テイカ製薬株式会社 | Granules for intraoral rapidly disintegrating tablets |
| WO2014059512A1 (en) | 2012-10-15 | 2014-04-24 | Isa Odidi | Oral drug delivery formulations |
| US20140275143A1 (en) | 2013-03-15 | 2014-09-18 | Mallinckrodt Llc | Compositions Comprising An Opioid And An Additional Active Pharmaceutical Ingredient For Rapid Onset And Extended Duration Of Analgesia That May Be Administered Without Regard To Food |
| US10420729B2 (en) | 2013-03-15 | 2019-09-24 | R.P. Scherer Technologies, Llc | Abuse resistant capsule |
| JP6445537B2 (en) | 2013-05-29 | 2018-12-26 | グリュネンタール・ゲゼルシャフト・ミト・ベシュレンクテル・ハフツング | Tamper-resistant dosage forms containing one or more particles |
| AR096439A1 (en) | 2013-05-29 | 2015-12-30 | Gruenenthal Gmbh | DOSAGE METHOD RESISTING TO INDEED USE CONTAINING ONE OR MORE PARTICLES |
| CA2817728A1 (en) | 2013-05-31 | 2014-11-30 | Pharmascience Inc. | Abuse deterrent immediate release formulation |
| EA032465B1 (en) | 2013-07-12 | 2019-05-31 | Грюненталь Гмбх | Tamper-resistant oral pharmaceutical dosage form containing ethylene-vinyl acetate polymer and process for the production thereof |
| US9770514B2 (en) | 2013-09-03 | 2017-09-26 | ExxPharma Therapeutics LLC | Tamper-resistant pharmaceutical dosage forms |
| WO2015048597A1 (en) | 2013-09-30 | 2015-04-02 | Daya Drug Discoveries, Inc. | Prevention of illicit methamphetamine manufacture from pseudoephedrine using food flavor excipients |
| US20150118300A1 (en) | 2013-10-31 | 2015-04-30 | Cima Labs Inc. | Immediate Release Abuse-Deterrent Granulated Dosage Forms |
| US10744131B2 (en) | 2013-12-31 | 2020-08-18 | Kashiv Biosciences, Llc | Abuse-resistant drug formulations |
| US10632113B2 (en) | 2014-02-05 | 2020-04-28 | Kashiv Biosciences, Llc | Abuse-resistant drug formulations with built-in overdose protection |
| CA2936565C (en) | 2014-02-12 | 2020-08-11 | Genentech, Inc. | Anti-jagged1 antibodies and methods of use |
| US20160089439A1 (en) | 2014-09-28 | 2016-03-31 | Satara Pharmaceuticals, LLC | Prevention of Illicit Manufacutre of Methamphetamine from Pseudoephedrine Using Food Flavor Excipients |
| JP6861646B2 (en) | 2015-02-05 | 2021-04-21 | グレイ オレンジ ピーティーイー. リミテッド | Equipment and methods for handling goods |
| EP3285745A1 (en) | 2015-04-24 | 2018-02-28 | Grünenthal GmbH | Tamper-resistant dosage form with immediate release and resistance against solvent extraction |
| US20170296476A1 (en) | 2016-04-15 | 2017-10-19 | Grünenthal GmbH | Modified release abuse deterrent dosage forms |
-
2010
- 2010-07-21 RU RU2012106166/15A patent/RU2555531C2/en not_active IP Right Cessation
- 2010-07-21 TW TW99123904A patent/TWI473628B/en not_active IP Right Cessation
- 2010-07-21 CA CA2767888A patent/CA2767888C/en not_active Expired - Fee Related
- 2010-07-21 PT PT107349243T patent/PT2456424E/en unknown
- 2010-07-21 EP EP10734924.3A patent/EP2456424B1/en active Active
- 2010-07-21 JP JP2012520952A patent/JP2012533586A/en active Pending
- 2010-07-21 KR KR1020127001863A patent/KR101747156B1/en active IP Right Grant
- 2010-07-21 MX MX2012000644A patent/MX2012000644A/en active IP Right Grant
- 2010-07-21 PL PL15184885T patent/PL2997965T3/en unknown
- 2010-07-21 PE PE2012000084A patent/PE20120631A1/en active IP Right Grant
- 2010-07-21 ES ES10734924T patent/ES2428938T3/en active Active
- 2010-07-21 ES ES15184885T patent/ES2718688T3/en active Active
- 2010-07-21 RU RU2015138422A patent/RU2015138422A/en unknown
- 2010-07-21 AR ARP100102650A patent/AR077420A1/en unknown
- 2010-07-21 NZ NZ596668A patent/NZ596668A/en not_active IP Right Cessation
- 2010-07-21 HU HUE15184885A patent/HUE042987T2/en unknown
- 2010-07-21 WO PCT/EP2010/004461 patent/WO2011009604A1/en active Application Filing
- 2010-07-21 KR KR1020127001831A patent/KR20120050975A/en active IP Right Grant
- 2010-07-21 US US12/840,471 patent/US20110020451A1/en not_active Abandoned
- 2010-07-21 MX MX2012000369A patent/MX2012000369A/en active IP Right Grant
- 2010-07-21 EP EP15184885.0A patent/EP2997965B1/en not_active Not-in-force
- 2010-07-21 PE PE2012000083A patent/PE20120572A1/en not_active Application Discontinuation
- 2010-07-21 ES ES10736630.4T patent/ES2560210T3/en active Active
- 2010-07-21 BR BR112012001244-4A patent/BR112012001244A2/en not_active Application Discontinuation
- 2010-07-21 PL PL10734924T patent/PL2456424T3/en unknown
- 2010-07-21 CN CN201080032917.XA patent/CN102573806B/en not_active Expired - Fee Related
- 2010-07-21 CN CN201080033849.9A patent/CN102639118B/en not_active Expired - Fee Related
- 2010-07-21 EP EP10736630.4A patent/EP2456425B1/en not_active Not-in-force
- 2010-07-21 SI SI201030332T patent/SI2456424T1/en unknown
- 2010-07-21 AU AU2010275754A patent/AU2010275754B2/en not_active Ceased
- 2010-07-21 BR BR112012001466-8A patent/BR112012001466A2/en not_active IP Right Cessation
- 2010-07-21 WO PCT/EP2010/004460 patent/WO2011009603A1/en active Application Filing
- 2010-07-21 RU RU2012106167/15A patent/RU2567723C2/en not_active IP Right Cessation
- 2010-07-21 AU AU2010275755A patent/AU2010275755B2/en not_active Ceased
- 2010-07-21 NZ NZ596666A patent/NZ596666A/en not_active IP Right Cessation
- 2010-07-21 JP JP2012520951A patent/JP2012533585A/en active Pending
- 2010-07-21 CA CA2766172A patent/CA2766172C/en not_active Expired - Fee Related
- 2010-07-21 EP EP13171574.0A patent/EP2662076A1/en not_active Withdrawn
-
2011
- 2011-11-22 IL IL216525A patent/IL216525A/en not_active IP Right Cessation
- 2011-11-22 IL IL216522A patent/IL216522A/en not_active IP Right Cessation
- 2011-11-22 CO CO11159567A patent/CO6470798A2/en not_active Application Discontinuation
- 2011-11-24 CL CL2011002970A patent/CL2011002970A1/en unknown
- 2011-11-24 CL CL2011002969A patent/CL2011002969A1/en unknown
- 2011-12-20 CO CO11175500A patent/CO6480912A2/en not_active Application Discontinuation
- 2011-12-21 ZA ZA2011/09446A patent/ZA201109446B/en unknown
- 2011-12-21 ZA ZA2011/09447A patent/ZA201109447B/en unknown
-
2012
- 2012-01-05 US US13/343,846 patent/US20120136021A1/en not_active Abandoned
- 2012-01-11 EC EC2012011591A patent/ECSP12011591A/en unknown
- 2012-01-11 EC EC2012011590A patent/ECSP12011590A/en unknown
- 2012-08-30 HK HK12108485.1A patent/HK1167810A1/en not_active IP Right Cessation
- 2012-08-30 HK HK12108484.2A patent/HK1167809A1/en not_active IP Right Cessation
- 2012-08-30 HK HK16104042.2A patent/HK1216296A1/en unknown
-
2014
- 2014-02-28 US US14/192,916 patent/US20140194455A1/en not_active Abandoned
-
2015
- 2015-09-01 US US14/841,829 patent/US9925146B2/en active Active
-
2017
- 2017-02-28 IL IL250841A patent/IL250841A0/en unknown
-
2018
- 2018-02-21 US US15/901,063 patent/US10493033B2/en active Active
-
2019
- 2019-10-15 US US16/653,186 patent/US20200038329A1/en not_active Abandoned
- 2019-12-03 US US16/701,921 patent/US20200101020A1/en not_active Abandoned
Also Published As
Similar Documents
| Publication | Publication Date | Title |
|---|---|---|
| US10493033B2 (en) | Oxidation-stabilized tamper-resistant dosage form | |
| US10064945B2 (en) | Thermoformed, tamper-resistant pharmaceutical dosage form containing zinc | |
| EP2846835B1 (en) | Thermoformed, tamper-resistant pharmaceutical dosage form containing zinc | |
| AU2013225106B2 (en) | Tamper-resistant dosage form comprising pharmacologically active compound and anionic polymer | |
| AU2012338872B2 (en) | Tamper-resistant oral pharmaceutical dosage form comprising a pharmacologically active ingredient, an opioid antagonist and/or aversive agent, polyalkylene oxide and anionic polymer | |
| NZ620252B2 (en) | Tamper-resistant oral pharmaceutical dosage form comprising opioid agonist and opioid antagonist | |
| NZ623291B2 (en) | Tamper-resistant oral pharmaceutical dosage form comprising a pharmacologically active ingredient, an opioid antagonist and/or aversive agent, polyalkylene oxide and anionic polymer |
Legal Events
| Date | Code | Title | Description |
|---|---|---|---|
| EEER | Examination request |
Effective date: 20150717 |
|
| MKLA | Lapsed |
Effective date: 20220301 |
|
| MKLA | Lapsed |
Effective date: 20200831 |