WO1999059573A1 - Stabilized pharmaceutical preparations of gamma-aminobutyric acid derivatives and process for preparing the same - Google Patents

Stabilized pharmaceutical preparations of gamma-aminobutyric acid derivatives and process for preparing the same Download PDF

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Publication number
WO1999059573A1
WO1999059573A1 PCT/US1999/010190 US9910190W WO9959573A1 WO 1999059573 A1 WO1999059573 A1 WO 1999059573A1 US 9910190 W US9910190 W US 9910190W WO 9959573 A1 WO9959573 A1 WO 9959573A1
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group
carbon atoms
acid
ring
amino
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PCT/US1999/010190
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French (fr)
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WO1999059573A9 (en
Inventor
Akira Aomatsu
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Warner Lambert Co LLC
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Warner Lambert Co LLC
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Priority to EP99924166A priority Critical patent/EP1077692B1/en
Priority to BRPI9910508-0A priority patent/BR9910508B1/en
Priority to IL13929899A priority patent/IL139298A0/en
Priority to SI9930624T priority patent/SI1077692T1/en
Priority to NZ508015A priority patent/NZ508015A/en
Priority to HU0102022A priority patent/HU228771B1/en
Priority to CA002327285A priority patent/CA2327285C/en
Priority to US09/674,815 priority patent/US7309719B1/en
Priority to DE69918977T priority patent/DE69918977T2/en
Application filed by Warner Lambert Co LLC filed Critical Warner Lambert Co LLC
Priority to PL344218A priority patent/PL204921B1/en
Priority to HK01107298.3A priority patent/HK1036586B/en
Priority to AT99924166T priority patent/ATE271864T1/en
Priority to AU40735/99A priority patent/AU768277B2/en
Publication of WO1999059573A1 publication Critical patent/WO1999059573A1/en
Publication of WO1999059573A9 publication Critical patent/WO1999059573A9/en
Priority to IS5666A priority patent/IS2233B/en
Priority to IL139298A priority patent/IL139298A/en
Priority to NO20005768A priority patent/NO328959B1/en
Anticipated expiration legal-status Critical
Ceased legal-status Critical Current

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    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/16Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing nitrogen, e.g. nitro-, nitroso-, azo-compounds, nitriles, cyanates
    • A61K47/18Amines; Amides; Ureas; Quaternary ammonium compounds; Amino acids; Oligopeptides having up to five amino acids
    • A61K47/183Amino acids, e.g. glycine, EDTA or aspartame
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/185Acids; Anhydrides, halides or salts thereof, e.g. sulfur acids, imidic, hydrazonic or hydroximic acids
    • A61K31/19Carboxylic acids, e.g. valproic acid
    • A61K31/195Carboxylic acids, e.g. valproic acid having an amino group
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/185Acids; Anhydrides, halides or salts thereof, e.g. sulfur acids, imidic, hydrazonic or hydroximic acids
    • A61K31/19Carboxylic acids, e.g. valproic acid
    • A61K31/195Carboxylic acids, e.g. valproic acid having an amino group
    • A61K31/197Carboxylic acids, e.g. valproic acid having an amino group the amino and the carboxyl groups being attached to the same acyclic carbon chain, e.g. gamma-aminobutyric acid [GABA], beta-alanine, epsilon-aminocaproic acid or pantothenic acid
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/06Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite
    • A61K47/20Organic compounds, e.g. natural or synthetic hydrocarbons, polyolefins, mineral oil, petrolatum or ozokerite containing sulfur, e.g. dimethyl sulfoxide [DMSO], docusate, sodium lauryl sulfate or aminosulfonic acids
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/20Pills, tablets, discs, rods
    • A61K9/2004Excipients; Inactive ingredients
    • A61K9/2013Organic compounds, e.g. phospholipids, fats
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/08Antiepileptics; Anticonvulsants
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/28Drugs for disorders of the nervous system for treating neurodegenerative disorders of the central nervous system, e.g. nootropic agents, cognition enhancers, drugs for treating Alzheimer's disease or other forms of dementia
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/14Particulate form, e.g. powders, Processes for size reducing of pure drugs or the resulting products, Pure drug nanoparticles
    • A61K9/16Agglomerates; Granulates; Microbeadlets ; Microspheres; Pellets; Solid products obtained by spray drying, spray freeze drying, spray congealing,(multiple) emulsion solvent evaporation or extraction
    • A61K9/1605Excipients; Inactive ingredients
    • A61K9/1617Organic compounds, e.g. phospholipids, fats

Definitions

  • This invention relates to a stabilized solid or liquid pharmaceutical preparation comprising a 4-a ino-3- substituted-butanoic acid derivative and a process for the preparation of the same.
  • the invention is concerned with a stabilized solid or liquid pharmaceutical preparation of the 4-amino-3-substituted-butanoic acid derivative, including gabapentin, pregabalin, baclofen, 3-aminomethyl-4- cyclohexyi-butanoic acid, 3-aminomethyl-5-cyclohe ⁇ yl pentanoic acid, 3-aminomethy -4-phenyl-butanoic acid or 3- aminomethyl-5-phenyl-pentanoic acid and a process for the preparation of the same.
  • the invention is concerned with a stabilized solid pharmaceutical preparation of a 4-amino- 3-substituted-butanoic acicj derivative, including gabapentin, pregabalin or baclofen, in the dosage forms of tablets, powders, granules and capsules and a stabilized liquid pharmaceutical preparation in the dosage forms of liquid preparations, syrups and injections, as well as a process for the preparation of the same.
  • a stabilized solid pharmaceutical preparation of a 4-amino- 3-substituted-butanoic acicj derivative including gabapentin, pregabalin or baclofen
  • Gabapentin easily passes across the brain barrier. Owing to this, the compound s used as a medicine for the treatment of certain cerebral diseases such as certain forms of epilepsy, faint and hypokin ⁇ sia as well as cranial traumas, and also for improving the cerebral functions in senile patients.
  • U.S. Patent No. 5,084,479 discloses that gabapentin is used for the treatment of neurodegenerative disorders such as Alzheimer's disease, Huntington's chorea or Parkinson's disease and amy ⁇ trophic lateral sclerosis.
  • U.S. Patent No. 5,025,035 discloses that gabapentin is used for the treatment of depression.
  • U.S. Patent No. 5,510,381 discloses that this compound is used for the treatment of mania and bipolar disorder.
  • this compound, having an analgesic activity is expected to be used as analgesics. Under these circumstances, there has been a greatly increased utility of gabapentin as the therapeutic agents for those diseases or disorders or conditions as recited above, m addition to cerebral diseases such as epilepsy and the like.
  • gabapentin is a very effective drug for cerebral diseases such as epilepsy and the like, and it has an extremely low toxicity.
  • it has been administered to adults usually at a single daily dose of 900 - 1800 mg or in some cases a daily dose of up to 2400 mg m three divided doses.
  • a single dose will be in the range of 300 - 600 mg or in some cases up to 900 mg .
  • gabapentin has difficulties in that it is a drug having a strongly bitter taste and also a very poor fluidity and that an extremely high dosage should be required for administration in the dosage form of powders. Since gabapentin is very difficult to formulate because of its instability, gabapentin capsules now available in the oversea markets are those manufactured by a simple dry blending of gabapentin with necessary auxiliaries and subsequent encapsulating into hard capsules. However, a single dose is as h gh as 300 - 600 mg or in some cases up to 800 mg as stated aoove, which necessitates large-sized capsules; for example, Capsule No .
  • gabapentin in its aqueous solution shows a very poor stability so that autodegra ⁇ ation may be easily brought about.
  • the mechanism of this autodegradation may be that the intramolecular condensation between the ammo group and the carboxyl group within the gabapentin molecule is caused through a dehydration reaction to form 4- cyclohexylvinylpyrrol d ⁇ ne (the corresponding lactam form) .
  • the autocondensation reaction rate may be variable depending upon storage temperature and can be far more accelerated as the temperature is elevated. Thus, this is the greatest reason why it has been difficult to manufacture a liquid pharmaceutical preparation of gabapentin.
  • gabapentin itself is a powdery material having very poor c ⁇ mpression- oldability and fluidity.
  • Compression molding or granulation has been usually employed for small- sizing or fluidizing drugs which have such powder properties, and these molding properties should be improved with the aid of pharmaceutical auxiliaries.
  • many of the auxiliaries to be applied for the purposes in accelerate the dehydration reaction between the amino group and the carboxyl group within the molecule of gabapentin to produce the corresponding lactam form, as the intramolecular condensation of gabapentin in its aqueous solution is accelerated.
  • an allowable content of the lactam up to the beyond-use date may be no more than 1.0% in view of safety. Accordingly, it is necessary in manufacturing a pharmaceutical preparation of gabapentin to prevent the formation of the lactam by retarding the dehydration reaction between the amino group and the carboxyl group within the molecule of gabapentin. On the other hand, it is a great problem to develop an adequate dosage form for easier ingesting, as discussed above.
  • ⁇ -aminobutyr ⁇ c acid derivatives having no or a less bulky substituent at the 3- position thereof such as ⁇ -ammobuty ⁇ c acid or 4-amino-3- hydroxy-butanoic acid
  • the dehydration reaction is not brought about even when maintained in a dried state such as at a temperature of 105°C over 2 - 3 hours, and the formation of 4-cyclohexylpyrrol ⁇ d ⁇ ne (the corresponding lactam form) is not observed.
  • the present invention relates to a stabilized pharmaceutical preparation containing a 4-amino-3-subst ⁇ tuted- butanoic acid derivative which comprises a 4-ammo-3- substituted-butanoic acid derivative having the general formula NH z CH ? -C-CH 2 COOH
  • R is a hydrogen atom, a hydroxyl group, a methyl group or an ethyl group
  • R 7 is a monovalent group selected from: a straight or branched alkyl group of 3 - 8 carbon atoms; a straight or branched alkylene group of 3-8 carbon atoms; a straight or branched alkyl group of 3 - ⁇ carbon atoms which is mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkyl group of 3 - 8 carbon atoms; a cycloalkyl group of 3 - 8 carbon atoms which is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an
  • -0-, -NH-, N-, -S-, -SO- or -S(0) 2 -, and one or two of the unsubstituted methylene groups (-CH 2 -) being mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CK 2 -) is replaced by -O-, -NH-, -S-, -SO- or -S(0) z -; a condensed ring group formed by ortho-fusion of a phenyl ring with
  • the invention also relates to a stabilized liquid pharmaceutical preparation containing a 4-amino-3- substituted-butanoic acid derivative.
  • the invention also relates to the stabilized liquid pharmaceutical preparation in the dosage form of liquid preparations, syrups QV injections.
  • the invention also relates to a stabilized solid pharmaceutical preparation containing a 4-amino-3- substituted-butanoic acid derivative.
  • the invention also relates to the stabilized solid pharmaceutical preparation in the dosage form of tablets, powders, granules or capsules.
  • the invention relates to a process for the preparation of a pharmaceutical preparation containing a 4- amino-3-5ubstituted-butanoic acid derivative which comprises combining a 4-amino-3-substituted-butano ⁇ c acid derivative having the following formula
  • R ⁇ and R 2 are as defined above
  • an amino acid as a stabilizer and, if necessary, an auxiliary agent for manufacturing a pharmaceutical preparation.
  • the invention further relats to a process for the preparation of a stabilized pharmaceutical preparation containing a 4-amino-3-substituted-butanoic acid derivative which is in a solid or liquid form.
  • the 4-amin ⁇ -3-subgtituted-butanoic acid derivatives which may be stabilized according to the present invention include those compounds as listed in the following
  • the present invention provides an extremely effective stabilizing means m manufacturing a pharmaceutical preparation containing a 4-am ⁇ no-3- substituted-butanoic acid derivative having a bulky substituent at the 3-posjt ⁇ n thereof as explained above, and the means of the invention is extremely effective in stabilizing these compounds m preparing a pharmaceutical preparation of, for example, gabapentin, pregabalin, baclofen, 3-am ⁇ nomethyl-4-cyclohe ⁇ yl-butan ⁇ c acid, 3- a ⁇ n ⁇ nomethyl-5-cyclohexyl-pentano ⁇ c ac d, 3-am ⁇ n ⁇ methyl-4- phenyl-butanoic acid, 3-aminomethyl-5-phenyl-pentano ⁇ c acid, etc .
  • the present invention relates to a stabilized pharmaceutical preparation containing a 4-ammo-3- substituted-butanoic acid derivative which comprises the 4- am ⁇ no-3-subst ⁇ tuted-butano ⁇ c acid derivative, an ammo acid as a stabilizer and, f necessary, an auxiliary agent for manufacturing a pharmaceutical preparation.
  • the invention also relates to a stabilized pharmaceutical preparation containing a 4-am ⁇ no-3- substituted-butanoic acid derivative m a liquid or solid form.
  • the invention also relates to a stabilized liquid pharmaceutical preparation containing a -ammo-3- substituted-butanoic acid derivative in the dosage form of liquid preparations, syrups or injections.
  • the invention also relates to a stabilized solid pharmaceutical preparation containing a 4-am ⁇ n ⁇ -3- substituted-butanoic acid derivative.
  • the invention also relates to a stabilized solid pharmaceutical preparation containing a -ammo-3- substituted-butan ⁇ ic ac d derivative in the dosage form of tablets, powders, granules or capsules.
  • the invention relates to a process for the preparation of a stabilized pharmaceutical preparation containing a 4-amino-3-subst ⁇ tuted-butanoic acid derivative which comprises combining the 4-a ⁇ mno-3-subst ⁇ tuted-butano ⁇ c ac d derivative with an ammo acid as a stabilizer and, if necessary, an auxiliary agent necessary for manufacturing a pharmaceutical preparation.
  • the invention relates to a process for the preparation of a stabilized pharmaceutical preparation containing a 4-ammo-3-subst ⁇ tuted-butano ⁇ c acid derivative which is in a solid or liquid form.
  • the pharmaceutical preparation containing a 4- ammo-3-subst ⁇ tuted-butano ⁇ c acid derivative stabilized by an ammo acid according to the invention nay be formulated into various dosage forms including liquid pharmaceutical preparations such as syrups or liquid preparations or solid pharmaceutical preparations such as powders, granules, capsules or tablets .
  • the assumed mechanism of action to stabilize a 4-amino-3-substituted-butanoic acid derivative with an amino acid is based upon the so-called "ion pair" theory that the carboxyl and amino groups commonly contained in an amino acid may form the corresponding ion pairs with the amino and carboxyl groups of the 4-amino-3-5Ubstituted-butanoic aci ⁇ derivative, respectively.
  • the present stabilization effect can not necessarily be accomplished by all sorts of amino acids.
  • the aminocarboxylic acid having an amino group at any position other than the ⁇ -position thereof such as the ⁇ -positi ⁇ n thereof, for example, ⁇ - alanine or, even of the ⁇ -amino acids, the amino acids having a pyrrolidine ring such as proline, hydroxyproline, etc. may show a weak stabilizing effect, while the ⁇ -amino acids having an amino group at the ⁇ -position thereof such as ⁇ -aminobutyric acid show no stabilizing effect.
  • the nmino acid which may be employed as an effective stabilizer ip the present invention is restricted to the ⁇ -amino acid having one free carboxyl group and one free amino group at the ⁇ -p ⁇ sition thereof.
  • all ⁇ -amino acids that have the said chemical structure can be used as a stabilizer in the present invention.
  • the ⁇ -ammo acid the present invention (also referred to as an ⁇ -monoammo-monocarboxylic acid) may be any of acidic ⁇ -ammo acids, basic ⁇ -amino acids, neutral ⁇ -amino acids and adducts of acidic ⁇ -amino acids with basic ⁇ -ammo acids.
  • the neutral ⁇ -amino acids may include glycme, phenylglycme, hydroxyphenylglycme, dihydroxyphenylglycine, L-alanine, hydroxy-L-alamne, -leucine, hydroxy- -leucme, dihydroxy-L-leucme, L-norleucme, methylene-L-norleucine, L-ketonorleucme, -isoleucine, hydroxy-L-isoleucine, dihydroxy-L-isoleucme, L-valine, hydroxy-L-valine, L- i ⁇ ovaline, L-norvalme, hyc$roxy- -norval ⁇ ne, hydroxy- - ketonorvaline, L-methionine ⁇ L-homomethionme, L-ethionine, -threonme, acetyl-L-threon e, L-tryptophan, hydroxy
  • the acidic ⁇ -amino acids may include I.-aspartic acid, L-glutamic acid, L-carbocysteine, L-amin ⁇ giutaric acid, L-aminosuccinic acid, L-aminoadiplc acid, L- aminopi elic acid, hydroxy-L-aminopimelic acid, methyl-L- aspartic acid # hydro ⁇ y-L-aspartic acid, methyl-L-glutamic acid, js ⁇ ethylhydroxy-L-glutamic acid, L-methyleneglutamic acid, hydroxy-L-glutamic acicj» dihydroxy-L-glutamic acid, hydroxy-L-aminoadipic acid ⁇ r the like and the D- and DL- forms thereof.
  • the basic ⁇ -ammo acids may include L-argmine, L- lys e, L-ornithme, L-canavanine, L-canalme, hydroxy-L- lysine, L-homoargmme, hydroxy-L-homoargmine, hydroxy-L- ornith e, L-diammopropionic acid, L-diammohexanoic acid, L-diaminobutyric acid, L-diammovaleric acid, L- diaminoheptanoic acid, L-di ii ⁇ inooctanoic ?c ⁇ d or the like and the D- and DL-forms thereof.
  • the ⁇ f ⁇ -dismmodicarboxylic acid may include diam osuccm c acid, diammogluta ⁇ c ac d, diammoadipic acid, diammopimelic acid or the like.
  • the acidic ⁇ -amino acid is used as a stabilizer for a 4-amino-3-_subst tuted-butano ⁇ c acid derivative in this invention
  • the ammo acid may be used in the form of an alkali salt thereof such as aspartic acid Na salt, aspartic acid K salt, glutamic acid Na salt, glutamic ac d K salt, aminopimelic acid Na salt, aminopimelic acid K salt or the like; an acid amide thereof such as asparagine, hydroxyasparagine, glutamine, hydroxyglutam e, metbyl ⁇ neglutamine or the like; an alkyl-substituted derivative of said acid amide such as methylasparagme, methyl
  • the amino acid may be used in the form of an acid addition salt thereof such as arginine hydrochloride, arginine acetate, lysine hydrochloride, lysine acetate, o nithine acetate or the like or a monoacylated derivative thereof such as acetyllysme, acetylornithme, acetylamino-aminobutyric acid, acetylamino- aminopropionic acid or the like.
  • an acid addition salt thereof such as arginine hydrochloride, arginine acetate, lysine hydrochloride, lysine acetate, o nithine acetate or the like or a monoacylated derivative thereof such as acetyllysme, acetylornithme, acetylamino-aminobutyric acid, acetylamino- aminopropionic acid or the like.
  • the acidic ⁇ -amino acid and the basic ⁇ -amino acid may be used in the form of the corresponding acidic amino acid-basic amino acid adduct such as aspartic acid • arginine, aspartic acid • lysine, aspartic acid • ornithine, glutamic acid • arginine, glutamic acid • lysine, or glutamic acid • ornithine adduct or the like.
  • ⁇ -amino acid Any of the ⁇ -amino acid mentioned above may be used alone or in combination with two or more thereof for liquid or solid pharmaceutical preparations of a 4-amino-3- ⁇ ubstituted-butanoic acid derivative.
  • the amino acid stabilizer of the invention may be blended with a 4-amino-3-substituted-butanoic acid derivative and then the resulting mixture may be simply dissolved in water to accomplish the object of stabilizing the 4-amino-3- substituted-butan ⁇ ic acid derivative; provided that the 4- amino-3-substituted-butanoic acid derivative to be used is limited solely to the m ⁇ noamino-monocarboxylic acid.
  • liquid pharmaceutical preparation for oral administration there may be incorporated, if required, a sweetening agent and/or a flavoring agent, which do not influence on the effect of the amino acid stabilizer.
  • amino acids may exert the effect as a stabilizer on injections or transfusions for which sterilization such as high pressure steam sterilization is required.
  • a wet admixture wherein a solution of the amino acid dissolved in a solvent such as water or the like is added to the 4-amino-3-substituted- butanoic acid derivative and a dry admixture wherein the amino acid in a dry state is added to the 4-amino-3- substituted-butanoic acid derivative.
  • the wet admixture of the amino acid may be carried out during the manufacture of a pharmaceutical preparation of a 4-amino-3-substituted-butanoic acid derivative, for example, in a wet granulation step wherein the amino acid in the form of its solution or suspension is added to bulk powders of the 4-amino-3-5Ubst ⁇ tuted-butanoic acid derivative together with a binder and an auxiliary agent for manufacturing a pharmaceutical preparation, or in a coating Step to apply a coating to granules or tablets for the purpose of masking a bittef tast wherein the amino acid is dissolved or suspended in _ ⁇ coating film base.
  • the wet granulation step of a 4-amino-3-' substituted-butanoic acid derivative may be carried out by adopting any granulation method well-known per __ ⁇ , for example, a fiuidized granulation method, a high speed stirring granulation method, a melting granulation method or the like.
  • a fluidized granulation method in which bulk powders of the 4-amino-3- substituted-butanoic acid derivative are fluidized and then a solution or suspension of a stabilizer and, if necessary, a binder and other auxiliary agents for manufacturing a pharmaceutical preparation may be sprayed on the fluidized powders .
  • granulation may be carried out by adding to bulk powders of a 4-amino-3- substituted-butanoic acid derivative the stabilizer solution as described above and, if necessary, a binder such as corn starch, a cellulose derivative (e.g., hydroxypropyl- cellulose) , p ⁇ lyvinyl alcohol, a polyvinyl pyrrolidone (e.g., Kollidon-K30 or Kollidon-K25) , a copolyvidone (e.g., Kollidon-VA64) and the like in the form of a solution or suspension thereof.
  • a binder such as corn starch, a cellulose derivative (e.g., hydroxypropyl- cellulose) , p ⁇ lyvinyl alcohol, a polyvinyl pyrrolidone (e.g., Kollidon-K30 or Kollidon-K25) , a copolyvidone (e.g., Kollidon-VA64) and the like in
  • the stabilizer may be added to bulk powders of the 4-amino-3-substituted-butano ⁇ c a-cid derivative by a wet or dry admixture up ⁇ .ng a bindr or other auxiliary agents for manufacturing a pharmaceutical preparation, and thereafter the granulation may be carried out.
  • a ' sweetening agent such as mannit ⁇ l, xylitol. sorbitol, aspartame and the like.
  • a polymeric base the form of a solution or suspension such as a cellulose derivative, e.g., hydroxypropylcellulose or hydroxypropylmethylcellulose, a polyvinyl yrrolidone, a copolyvidone, Eudragits and the like and, if necessary, a sweetening agent such as mannitol, xylitol, sorbitol, aspartame or the like.
  • Sur ce-coating of granules or tablets may be carried out by a well-known method using a fluidized bed or a rotary pan.
  • the dry admixture of the ammo acid may be carried out, beside the dry admixture in the aforementioned wet granulation step, a mixing step of powders prepared, for example, for compression using a tablet machine, for filling into hard capsules using a capsule filling machine or for filling using a distribution machine or the like.
  • t is preferable to use L-leucme, L-isoleucme, L-valme, D-leuci ⁇ e, D- is ⁇ leucme, D-valme, DL-leucme, DL-isoleucme or DL-valme.
  • the ammo acid may be usually blended with, as required, an auxiliary agent for manufacturing a pharmaceutical preparation, for example, a binder or a disintegrator such as a cellulose derivative, e.g., hydroxypropylcellulose, crystalline cellulose, corn starch, partially gelatinized starch or lactose or the like and/or ⁇ sweetening agent such as mannitol, xylitol, sorbitol, aspartame or the like by means of a suitable mixer such as a well-known dry mixer, e.g., a V-blender or the like.
  • a binder or a disintegrator such as a cellulose derivative, e.g., hydroxypropylcellulose, crystalline cellulose, corn starch, partially gelatinized starch or lactose or the like and/or ⁇ sweetening agent such as mannitol, xylitol, sorbitol, aspartame or the like by means of a suitable mixer such
  • the solid pharmaceutical preparation of a 4- m ⁇ no- 3-3ubstituted-kutano ⁇ c aci ⁇ derivative which has been stabilized by the addition of the ammo acid can be formulated the compressed dosage form of, for example, tablets or the fluidized dosage form of, for example, - 53
  • the resulting dosage form may be easily ingested when orally administered to human.
  • the solid pharmaceutical preparation when administered in the form of an aqueous solution or suspension thereof, for example, the case of dry syrups or effervescent tablets as dissolved or suspended m water, a stabilizing effect may be accomplished as in the case of the liquid pharmaceutical preparation.
  • the pharmaceutical preparation of a 4-am no-3-subst ⁇ tuted-butanoic acid derivative of the invention includes both of liquid and solid pharmaceutical preparations and a total amount of the ammo acid as a stabilizer in a liquid pharmaceutical preparation may be in the range of 0.005 - 80 moles, preferably 0.01 - 70 moles, per 1 mole of the 4-am ⁇ no-3-subst ⁇ tuted-butano ⁇ c acj d derivative, and in a solid pharmaceutical preparation, it may be in the range of 0.001 - 80 moles.
  • the amino acid may preferably be used the amount as defined above, the amount may vary depending upon the dosage form, a sort of the auxiliary agent to be used as well as the amount thereof to be blended.
  • the amino ac d when used beyond the upper limit would not noticeably lower or vitiate its effect.
  • the upper limit of the amount to be blended is not limited to the application range as defined above.
  • the said preparation is in the form of a solid pharmaceutical preparation
  • Example 1 In this Example, the following Samples (a) , (b) and (c) of aqueous solutions of gabapentin were tested for stability.
  • Sample (a) was prepared by dissolving 500 mg of gabapentin crystals in water to make up a total volume of 10 ml.
  • Sample (b) was prepared by dissolving 500 mg of gabapentin crystals and 329 mg of glycine water to make up a total volume of 10 ml.
  • Sample (c) was prepared by dissolving 500 mg of gabapentin crystals and 513 mg of L-valine in water to make up a total volume of 10 ml.
  • Example 2 In this Example, the following Samples (d) , (e) and (f) of aqueous solutions of gabapentin were tested for stability.
  • Sample (d) was prepared by dissolving 500 mg of gabapentin crystals in ate ⁇ to make up a total volume of 10 pil.
  • Sample (e) was prepared by dissolving 500 mg of gabapentin crystals and 1.5 g of xylitol in water to make up a total volume of 10 ml.
  • Sample (f) was prepared by dissolving 500 mg of gabapentin crystals, 219 mg of glycine and 1.5 g of xylitol in water to make up a total volume of 10 ml.
  • Example 3 In this Example, the following Samples (g) and (h) of aqueous solutions of gabapentin were tested for stability. Preparation of samples:
  • Sample (g) was prepared by dissolving 10 g of gabapentin crystals in water to make up a total volume of 200 ml.
  • Sample (h) was prepared by dissolving 25 g of gabapentin crystals, 8.25 g of glycine, 9.75 g of DL- alanine, 100 g of xylitol and 0.05 g of perfume in water to make up a total volume of 500 ml.
  • pe ples (i) and (j) of gabapentin granules were prepared as follows: 1) Using a fluidized bad granulation apparatus, 72 g of water was sprayed onto 250 g of gabapentin crystals and successively a solution prepared by dissolving 5 g of hydroxypropylcellulose in 56 g of water was sprayed thereon and the product was dried to form Sample (i) of gabapentin granules.
  • the gabapentin granules prepared as described abovg were compressed to form tablets, each having a weight of 20 ⁇ mg, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 2 - 3 kg, which were used as Sample (1) .
  • the gabapentin granules prepared as described the above 1) were admixed with L-isoleucine at 2?, by weight relative to the granules and then compressed using a rotary tablet machine to form tablets, each having a weight of 208 rag, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 4 - 5 kg, which were used as Sample (n) .
  • Example 6 This Example will illustrate the preparation of a stabilized solid pharmaceutical preparation of gabapentin by the addition of the amino acid to gabapentin according to the dry admixture.
  • Example B In this Example, the following samples (t) , (u) and (v) were tested for stability in aqueous solutions of pregabalin.
  • Sample (u) was prepared by dissolving 1 g of pregabalin crystals and 0.94 g of glycine in water to make up a total volume of 50 ml.
  • Sample (v) was prepared by dissolving 1 g ⁇ f pregabalin crystals and 1.47 g ⁇ f L-valine in water to make up a total volume of 50 ml .
  • Samples (t) , !u) md (v) prepared as described above were stored under the conditions as defined, in the following Table 10 and then a content of the dehydrated condensate formed in each ⁇ f the aqueous solutions was determined by means of HPLC. In this Example and the following Examples, a content of the dehydrated condensate formed is expressed in terms of % by weight, based on pregabalin. Table 10
  • Sample (aa) of pregabalin granules and Samples (ab) , i ⁇ c) and (ad) of pregabalin tablets were prepared as follo s: Preparation of samples: 1) 1 g of pregabalin crystals was prepared to powdery Sample (aa) m a compacted state by means of a mortar.
  • Samples (aa) , (ab) , (ac) and (ad) prepared as described above and untreated pregabalin crystals were stored under the conditions as defined in the following Table 11 and then a content o the dehydrated condensate formed in each ⁇ f the samples was determined by means of HPLC.
  • Example 10 In this Example, the following Samples (ae) and (af) were tested for stability in aqueous solutions of baclofen. Preparation of samples:
  • Sample (ae) was prepared by dissolving 0.05 g of baclofen crystals in water to make up a total volume ⁇ f 50 ml
  • Sample (af) was prepared by dissolving 0.0b g of baclofen crystals and 0.05 g of glycine in water to make up a total volume of 50 ml.
  • a content of the dehydrated condensate thus formed is expressed in terms of % by weight, based en baclofen. - 73
  • baclofen could be prevented from the degradation with lapse of time (the condensation with dehydration) in its aqueous solution by the addition of glycine under all the storage and heating conditions.
  • Sample (ah) was prepared by wetting 200 mg of baclofen crystals with 0.1 ml of a 2% aqueous solution of L- isoleuc e, forming granular powders by means ⁇ f a mortar and then drying.
  • the stabilization of a pharmaceutical preparation containing a 4-ammo-3-subst ⁇ tuted-butano ⁇ c acid derivative can be accomplished by the additicn of an am o acid.
  • the stabilization by the addition of an am o acid can be accomplished not only in solid pharmaceutical preparations but also in liquid pharmaceutical preparations, stabilization of which has not been succeeded.
  • he present invention can provide diverse means to administer a pharmaceutical preparation of a 4-ammo-3-tsubst ⁇ tuted- butanoic acid derivative; for example, he 'difficulty encountered in the prior art when admm ⁇ st
  • the present invention can be expected to greatly contribute to the development of a stabilized pharmaceutical preparation of a 4-ammo-3- substituted-butanoic acid deriva e.

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Abstract

The present invention provides a stabilized pharmaceutical preparation of a 4-amino-3-substituted-butanoic acid derivative which can be obtained by incorporating an amino acid as a stabilizer.

Description

STABILIZED PHARMACEUTICAL PREPARATIONS OF GAMMA-AMINOBUTYRIC ACID DERIVATIVES AND PROCESS FORPREPARING THE SAME
FIELD OF THE INVENTION
This invention relates to a stabilized solid or liquid pharmaceutical preparation comprising a 4-a ino-3- substituted-butanoic acid derivative and a process for the preparation of the same. Particularly, the invention is concerned with a stabilized solid or liquid pharmaceutical preparation of the 4-amino-3-substituted-butanoic acid derivative, including gabapentin, pregabalin, baclofen, 3-aminomethyl-4- cyclohexyi-butanoic acid, 3-aminomethyl-5-cycloheκyl pentanoic acid, 3-aminomethy -4-phenyl-butanoic acid or 3- aminomethyl-5-phenyl-pentanoic acid and a process for the preparation of the same.
More particularly, the invention is concerned with a stabilized solid pharmaceutical preparation of a 4-amino- 3-substituted-butanoic acicj derivative, including gabapentin, pregabalin or baclofen, in the dosage forms of tablets, powders, granules and capsules and a stabilized liquid pharmaceutical preparation in the dosage forms of liquid preparations, syrups and injections, as well as a process for the preparation of the same.
BACKGROUND OF THE INVENTION 1- (Aminomethyl) cyclσhexaneacetic acid, one of the
4-amino-3-substituted-butanoιc acid derivatives, having the following structural formula is disclosed m U.S. Patent Nos. 4,024,175 and 4,087,544 and has been called "gabapentin", a generic name, due to its structural relation to γ-ammobutyrιc acid (GABA) .
Figure imgf000004_0001
Gabapentin easily passes across the brain barrier. Owing to this, the compound s used as a medicine for the treatment of certain cerebral diseases such as certain forms of epilepsy, faint and hypokinβsia as well as cranial traumas, and also for improving the cerebral functions in senile patients.
Moreover, U.S. Patent No. 5,084,479 discloses that gabapentin is used for the treatment of neurodegenerative disorders such as Alzheimer's disease, Huntington's chorea or Parkinson's disease and amyσtrophic lateral sclerosis. U.S. Patent No. 5,025,035 discloses that gabapentin is used for the treatment of depression. U.S. Patent No. 5,510,381 discloses that this compound is used for the treatment of mania and bipolar disorder. Furthermore, this compound, having an analgesic activity, is expected to be used as analgesics. Under these circumstances, there has been a greatly increased utility of gabapentin as the therapeutic agents for those diseases or disorders or conditions as recited above, m addition to cerebral diseases such as epilepsy and the like.
As stated above, gabapentin is a very effective drug for cerebral diseases such as epilepsy and the like, and it has an extremely low toxicity. However, in order to maintain the effect as expected, it has been administered to adults usually at a single daily dose of 900 - 1800 mg or in some cases a daily dose of up to 2400 mg m three divided doses. Thus, a single dose will be in the range of 300 - 600 mg or in some cases up to 900 mg .
Further, gabapentin has difficulties in that it is a drug having a strongly bitter taste and also a very poor fluidity and that an extremely high dosage should be required for administration in the dosage form of powders. Since gabapentin is very difficult to formulate because of its instability, gabapentin capsules now available in the oversea markets are those manufactured by a simple dry blending of gabapentin with necessary auxiliaries and subsequent encapsulating into hard capsules. However, a single dose is as h gh as 300 - 600 mg or in some cases up to 800 mg as stated aoove, which necessitates large-sized capsules; for example, Capsule No . 0 snould be applied to capsules having a content of 400 mg per capsule. Consequently, ingesting such capsules is difficult even for adults, much more for children. Although gabapentin capsules have already been marketed, it is still indispensable to attempt any improvement m compliance and easy administration of gabapentin, and a αemand for a smaller-sized pharmaceutical preparation of gabapentin exists in the clinical field.
However, gabapentin in its aqueous solution shows a very poor stability so that autodegraαation may be easily brought about. The mechanism of this autodegradation may be that the intramolecular condensation between the ammo group and the carboxyl group within the gabapentin molecule is caused through a dehydration reaction to form 4- cyclohexylvinylpyrrol dσne (the corresponding lactam form) . In this regard, the autocondensation reaction rate may be variable depending upon storage temperature and can be far more accelerated as the temperature is elevated. Thus, this is the greatest reason why it has been difficult to manufacture a liquid pharmaceutical preparation of gabapentin.
On the other hand, another reason for difficulty in manufacruring a pharmaceutical preparation of gabapentin lies in that gabapentin itself is a powdery material having very poor cσmpression- oldability and fluidity. Compression molding or granulation has been usually employed for small- sizing or fluidizing drugs which have such powder properties, and these molding properties should be improved with the aid of pharmaceutical auxiliaries. However, many of the auxiliaries to be applied for the purposes in accelerate the dehydration reaction between the amino group and the carboxyl group within the molecule of gabapentin to produce the corresponding lactam form, as the intramolecular condensation of gabapentin in its aqueous solution is accelerated. This dehydration reaction would be far more accelerated as the gabapentin powder is being more tightly compressed. Moreover, the reaction between gabapentin and such auxiliaries with lapse of time would be further accelerated by the use of water or an organic solvent in manufacturing a pharmaceutical preparation.
In short, it has been elucidated that the degradation of gabapentin with lapse of time due to the formation of the lactam is the phenomenon which shall be ascribed to the chemical structure of gabapentin itself and developed by the influence of water, irrespective of whether or not gabapentin is in the state of a solution or a solid.
It has been standardized m commercially available gabapentin capsules that an allowable content of the lactam up to the beyond-use date may be no more than 1.0% in view of safety. Accordingly, it is necessary in manufacturing a pharmaceutical preparation of gabapentin to prevent the formation of the lactam by retarding the dehydration reaction between the amino group and the carboxyl group within the molecule of gabapentin. On the other hand, it is a great problem to develop an adequate dosage form for easier ingesting, as discussed above.
Thus, in order to prepare a liquid pharmaceutical preparation of gabapentin, there have been made studies on, for example, controlling of pH, controlling of activity of water. Also, there have been attempted various methods, in order to form a smaller-sized solid pharmaceutical preparation of gabapentin. However, all of these prior art - 7 -
methods to manufacture solid or liquid preparations of gabapentin have not yet succeeded due to the presence of the lactam form found as the results of stability tests.
Because of this, a pharmaceutical preparation of gabapentin now commercially available is limited to large-sized hard capsules only, although there has been a continuous need from the clinical field.
Such instability as encountereα n manu acturing a gabapentin preparation has been also observed in other 4- amino-3-substituted-butanoιc acid derivatives which are structurally analogous to gabapentin and have a structurally bulky substituent at the 3-positiσn thereof similarly to gabapentin.
For example, 4-amino-3-p-chlorophenyl) butanoic acid, which is represented by the following structural formula and called "baclofen" m a generic name,
Figure imgf000009_0001
and 5-methyl-3-aminomethyl-hexanoic acid, which is represented._by the following structural formula and called "pregabalin" in a generic name,
Figure imgf000010_0001
are also a drug which has very poor compression-moldability and fluidity like gabapentin. Compression molding or granulation used for small-sizing or fluidizing the drug should be improved with the aid of pharmaceutical auxiliaries. However, many of the auxiliaries to be applied to compression molding tend to react with gabapentin with lapse of time to form 4-cyclσhexylpyrrolidone (the corresponding lactam form) by accelerating the dehydration reaction between the amino group and the carboxyl group withm the molecule of the compound. This dehydration reaction would be far more accelerated as the compound is being more tightly compressed and would be further accelerated by the use of water or an organic solvent in manufacturing a pharmaceutical preparation, as is the case of gabapentin. It may be said that the mechanism of degradation by the autocondensation is peculiar to the 4- amιno-3-5ubstituted-butanoie acid derivatives having a structurally bulky substituent at the 3-position thereof.
To the contrary, in γ-aminobutyrιc acid derivatives having no or a less bulky substituent at the 3- position thereof, such as γ-ammobutyπc acid or 4-amino-3- hydroxy-butanoic acid, the dehydration reaction is not brought about even when maintained in a dried state such as at a temperature of 105°C over 2 - 3 hours, and the formation of 4-cyclohexylpyrrolιdσne (the corresponding lactam form) is not observed. In other words, in the 4-ammσ-3- substituted-butanσic acid derivative wherein the substituent at the 3-posιtισn thereof has a bulky structure, the dehydration reaction could easily be brought about between the ammo group and the carboxyl group within the molecule.
In view of the aforesaid background, for drugs which are 4-amιno-3-substituted-butanoιc acid derivatives, including gabapentin, having a structurally bulky substituent at the 3-posιtιon thereof, there have been desired a new pharmaceutical preparation containing said drugs which has an excellent storage stability in the form of liquid preparations or in a small-sized or fluidized dosage form such as tablets or granules for easier mgestion and a process for manuf cturing the same.
SUMMARY Of THE INVENTION We have made earnest studies to solve the prior art problems as stated above and, as a result, have now found that the lactam formation through the intramolecular condensation can be prevented by blocking both the ammo group and carboxyl group of a 4-amino-3-substιtuted-butano c acid derivative, that it is effective for blocking the am o and carboxyl groups of the 4-amιno-3-substιtuted-butanoιc acid derivative to add as a stabilizer an amino acid having a carboxyl group and an amino group with its molecule to the 4-ammo-3-substιtuted-butanoιc acid derivative, and that the 4-ammo-3-substιtuted-butanoic acid derivative can possess a superior storage stability not only the form of its aqueous solution but also in a solid state, on the basis of which this invention has been completed.
DETAILED DESCRIPTION OF THE INVENTION The present invention relates to a stabilized pharmaceutical preparation containing a 4-amino-3-substιtuted- butanoic acid derivative which comprises a 4-ammo-3- substituted-butanoic acid derivative having the general formula NHzCH?-C-CH2COOH
/ \
wherein, R, is a hydrogen atom, a hydroxyl group, a methyl group or an ethyl group;
R7 is a monovalent group selected from: a straight or branched alkyl group of 3 - 8 carbon atoms; a straight or branched alkylene group of 3-8 carbon atoms; a straight or branched alkyl group of 3 - θ carbon atoms which is mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkyl group of 3 - 8 carbon atoms; a cycloalkyl group of 3 - 8 carbon atoms which is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho- fusion of a phenyl ring with a cycloalkyl group of 4 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 4 - 8 carbon atoms wherein said phenyl ring is mono-, di- or tri-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkeπyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms wherein said phenyl ring is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; an alkylcycloalkyl qrσup wherein said cycloalkyl has
3 - 8 carbon atoms and is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -S- or -SS-; an alkylcycloalkyl group wherein said cycloalkyl has 3 - 8 carbon atoms, is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0~, -5- or -SS- and s mono-, di- or tri-substituted with a halogen atom," a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CHZ-) is replaced by -0-, -NH-, -S-, -SO- or -S(0)2-; a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH2-) is replaced by -O-, -NH-, -S-, -SO- or -S(0)2-, and one or two of the unsubstituted methylene groups {-CH7-) are mono- or di-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an ammo group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH2-) in (said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, =N-, -S-, -SO- or -S(0)2-; a cycloalkenyl group of 5 - 8 carbon atoms or e cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH2-) in said cycloalkenyl ring or cycloalkanedienyϊ ring being replaced by. -0-, -NH-, =N-, -S-, -SO- or -S(0)2-, and one or two of the unsubstituted methylene groups (-CH2-) being mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CK2-) is replaced by -O-, -NH-, -S-, -SO- or -S(0)z-; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH,-) is replaced by -O-, -NH-, -5-, -50- or -5(0)2-, said phenyl group being mono- or di-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH.,-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, =N-, -S-, -SO- or -S(0)2-; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH2-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, =N-, -S-, -SO- or -S(0)2-, said phenyl ring being mono- or di-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; an alkylcycloalkyl group wherein said cycloalkyl has 5 - 8 carbon atoms and is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -S- or -SS-, one of the methylene groups (-CH2-) in said cycloalkyl ring being replaced by -Q-, -NH-, -5-, -SO- or -S(0)2-; an alkylcycloalkyl group wherein said cycloalkyl has 5 - 8 carbon atoms and is lin ed to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -5- or -SS-, and one of the methylene groups (-CH2-) in said cycloalkyl ring being replaced by -O-, -NH-, -S-, -SO- or -S(0)2- and one or two of the unsubstituted methylene groups (-CH2-) being mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a phenyl or naphthyl group; a phenyl group substituted with a methylenediσxy group; a phenyl or naphthyl group which is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group, a carboxyl group, a phenoxy group, a phenylmethoxy group, a phenylmethoxy group wherein said phenyl rmg is mono-substituted with a halogen atom, trifluoromethyl group, an alkoxy group, an ammo group, a nitro group, a carboxyl group or a carboalkoxy group, a cycloalkylmethoxy group having 5 - 8 carbon atoms in the cycloalkyl ring, a cycloalkenylmethoxy group having 5 - B carbon atoms in the cycloalkenyl rmg, a cycloalkanedienylmethoxy group having 5 - 8 carbon atoms in the cycloalkanedienyl ring, • cycloalkylmethoxy group wherein one of the methylene groups (-CH-.-) in said cycloalkyl rmg having 5 - 8 carbon atoms is replaced by -0-, -NH-, -S-, -SO- or -S(0)j-, a cycloalkenylmethoxy group wherein one of the methylene groups (-CH--) in said cycloalkenyl ring having 5 - 8 carbon atoms is replaced by -O-, -NH-, =N-, -S-, -50- or -S(0)2~, a cycloalkanedienyl- methoxy group wherein one of the methylene groups (-CH2-) in said cycloalkanedienyl ring having 5 - 8 carbon atoms is replaced by -O-, -NH-, =N-, -S-, -SO- or -S(0)2- group, a cycloalkylmethoxy group having 5 - 8 carbon atoms in the cycloalkyl ring wherein said cycloalkyl ring is mono-substituted with a halogen atom, trifluoromethyl group, a hydroxy group, an alkyl group, an alkoxy group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH2-. in said cycloalkyl ring is replaced by -O-, -NH-, -5-, -SO- or -S(0)2-, a cycloalkenylmethoxy group having 5 - 8 carbon atoms in the cycloalkenyl ring wherein said cycloalkenyl ring is mono-substituted with a halogen atom, a trifluoromethyl group, a hydroxy group, an alkyl group, an alkoxy group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH-) in βaid cycloalkenyl ring is replaced by -O-, -NH-, =N-, -S-, -SO- or -5(0)2-, or a cycloalkanedienylmethoxy group having 5 - 8 carbon atoms in the cycloalkanedienyl ring wherein said cycloalkanedienyl ring is mono-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH--) in said cycloalkanedienyl ring is replaced by -O-, -NH-, -N-, -S-, -SO- or -S(0).-; an alkylphenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O-, -5- or -S5-; an alkyl-O-, -5- or -SS-phenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms via -o-, -S- or -S5-; an -0-, -5- or -SS-phenyl group; a diphenylamino group: an alkylphenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O-, -S- or -55- and mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, a alkyl group, an alkoxy group, an amino group, a nitro group βr a carboxyl group; an alkyl-O-, -S- or -SS-phenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms via -O-, -S- or -SS- and mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; an -O-, -5- or -SS-phenyl group wherein said phenyl group is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a nydroκyl group, an alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; or n and R2, together with the carbon atom to which they are attached, may form a divalent group selected from: a cycloalkylidene group of 5 - 8 carbon atoms; a cycloalkylidene group of 5 - θ carbon atoms which is mono-, di-, tri- or tetr-i-substituted with a halogen atom, a trifluoromethyl group* a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, a cycloalkyl group, a phenyl group, an anino group, a nitro group or a carboxyl group; a cycloalkylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH2-) in said cycloalkyl ring is replaced by -0-, -NH-, -S-, -SO- or -S(0)2-; a cycloalkylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH2-) in said cycloalkyl ring is replaced by -0-, -NH-, -S-, -SO- or -S(0) - group and one or more of the unsubstituted methylene groups (-CHZ-) in said cycloalkyl ring are mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms; a cycloalkenylidene group of 5 - 3 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms which is mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, a cycloalkyl group, a phenyl group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenylidene group of 5 - θ carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms wherein one of the methylene groups ,-CH2-) in said cycloalkenyl ring or cycloalkanedienyl ring is replaced by -O-, -NH-, =N-, -S-, -So- or -S(O) 2-; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH-) in said cycloalkenyl ring or cycloalkanedienyl ring is replaced by -O-, -NH-, =N-, -S-, -SO- or -S (o) 2- group and one or more of the unsubstituted methylene groups (-CH2-) in said cycloalkenyl ring or cycloalkanedienyl ring are mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkylidene group of 4 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkylidene group of 4 - 8 carbon atoms, said phenyl ring being mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an al yl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms , said phenyl ring being mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; an α-amino acid; and, if necessary, an auxiliary agent for manufacturing a pharmaceutical preparation.
The invention also relates to a stabilized liquid pharmaceutical preparation containing a 4-amino-3- substituted-butanoic acid derivative.
The invention also relates to the stabilized liquid pharmaceutical preparation in the dosage form of liquid preparations, syrups QV injections.
The invention also relates to a stabilized solid pharmaceutical preparation containing a 4-amino-3- substituted-butanoic acid derivative. The invention also relates to the stabilized solid pharmaceutical preparation in the dosage form of tablets, powders, granules or capsules.
Also, the invention relates to a process for the preparation of a pharmaceutical preparation containing a 4- amino-3-5ubstituted-butanoic acid derivative which comprises combining a 4-amino-3-substituted-butanoιc acid derivative having the following formula
NH-CH--C-CH2CO0H
/ \
(wherein Rλ and R2 are as defined above) with an amino acid as a stabilizer and, if necessary, an auxiliary agent for manufacturing a pharmaceutical preparation.
The invention further relats to a process for the preparation of a stabilized pharmaceutical preparation containing a 4-amino-3-substituted-butanoic acid derivative which is in a solid or liquid form.
The 4-aminσ-3-subgtituted-butanoic acid derivatives which may be stabilized according to the present invention include those compounds as listed in the following
Tables 1 and.'2: - 74
Table 1 zCOOH
Figure imgf000026_0001
Figure imgf000026_0002
-H -CH(CH3)2
-H -CH2-CHZ-CH2-CH3 -H ^D
Figure imgf000026_0003
-H -(CHZ),-CHS
-H -(CHa)3-CH-(CH,)8 -H
-H -CH(CHZ-CH3)(CHS)
-H -CH.-CHj-CHiNI -H
Figure imgf000026_0004
-H -CH2-CH2-CHz-CH2-NHz
Figure imgf000026_0005
-H -CHz-CHz-CH2-CH0H -H
Figure imgf000026_0007
Figure imgf000026_0006
Table 1 (Cont'd) NHzCH2-C-CHzCOOH tf z
Figure imgf000027_0001
-H -CH; -H -ώ Table 1 ( Con 'd)
NH zCOOH
Figure imgf000028_0001
Figure imgf000028_0002
-H -H i^^S ) \ 1
Figure imgf000028_0003
Table 1 (Cont'd)
Figure imgf000029_0001
Table 1 (Cont'd) NH2CHz-C-CHzC00H
Figure imgf000030_0001
- 7.9
Table 1 (Cont'd)
Figure imgf000031_0001
Table 1 (Cont'd)
Figure imgf000032_0001
Figure imgf000032_0002
Figure imgf000032_0003
Table 1 (Cont'd)
Figure imgf000033_0001
Figure imgf000033_0002
Figure imgf000033_0003
Table 1 (Cont'd)
NH2CH 2C00H
Figure imgf000034_0001
Figure imgf000034_0002
— CH2-CHZ- -H -o NH,
-H -CHz-0-CHz -H -<O
Figure imgf000034_0003
Table 1 (Cont'd)
NH2 CHz-( :-CH aCOOH \ R. Rz
Figure imgf000035_0001
-H -H -O nPro
Figure imgf000035_0002
-H /~C?- -H -OMe
Figure imgf000035_0003
-H -^_ ~*e -H -O OH
Figure imgf000035_0004
Table 1 (Cont'd)
NH
Figure imgf000036_0001
-R -Rz -R. -R>
Figure imgf000036_0002
OMe
-H
^=> -o
Figure imgf000036_0003
-H — J — OiPro -H -CH2-0-CH2 -o
Figure imgf000036_0004
Table 1 .Cont'd)
Figure imgf000037_0001
-H -CH3-CH»-0-CHz→Q-NH2 -H -s-O01
Figure imgf000037_0002
-H -CHz-CH2-S-CIIrQ>-Br
Figure imgf000037_0003
Table 2
NHjCHz-C- CH»C OOH R, Ra
Figure imgf000038_0001
Table 1 (Cσi nt* d)
NHZCHZ-C-CH zCOOH
Figure imgf000039_0001
-H -CH-CH-CHz-CHs -H -CH=CH-CH(CH3)z
-H -C(CH3)=CΠ-CH3
-H -CΠ=C(CH3)2
Table 1 (Cont'd)
NH? CHa-C-CH»C00H Ri R2
Figure imgf000040_0001
-OH -CHZ-C(CH3)J -CHj -CH(CH3)z
-OH -CH2-CH2-CH3 -CHj -CHz-CH(CH3)z
-OH -CH2-CH2-CH2-CH3 -CH3 -CH j — CH j — H 2 -CH 3
-OH -
-OH
-OH
-OH
-OH
Figure imgf000040_0002
Figure imgf000040_0003
Table 2 (Cont'd)
NH,CH,-C-CH,COOH R. ,
Figure imgf000041_0001
Table 2 (Cont'd)
Figure imgf000042_0001
R.
>c< > ;
Figure imgf000042_0002
Table 2 (Cont'd) NH2CH, HjCOOH
Figure imgf000043_0001
Figure imgf000043_0002
The present invention provides an extremely effective stabilizing means m manufacturing a pharmaceutical preparation containing a 4-amιno-3- substituted-butanoic acid derivative having a bulky substituent at the 3-posjtισn thereof as explained above, and the means of the invention is extremely effective in stabilizing these compounds m preparing a pharmaceutical preparation of, for example, gabapentin, pregabalin, baclofen, 3-amιnomethyl-4-cycloheκyl-butanαιc acid, 3- aιnιnomethyl-5-cyclohexyl-pentanoιc ac d, 3-amιnαmethyl-4- phenyl-butanoic acid, 3-aminomethyl-5-phenyl-pentanoιc acid, etc .
The present invention relates to a stabilized pharmaceutical preparation containing a 4-ammo-3- substituted-butanoic acid derivative which comprises the 4- amιno-3-substιtuted-butanoιc acid derivative, an ammo acid as a stabilizer and, f necessary, an auxiliary agent for manufacturing a pharmaceutical preparation.
The invention also relates to a stabilized pharmaceutical preparation containing a 4-amιno-3- substituted-butanoic acid derivative m a liquid or solid form. The invention also relates to a stabilized liquid pharmaceutical preparation containing a -ammo-3- substituted-butanoic acid derivative in the dosage form of liquid preparations, syrups or injections. The invention also relates to a stabilized solid pharmaceutical preparation containing a 4-amιnσ-3- substituted-butanoic acid derivative.
The invention also relates to a stabilized solid pharmaceutical preparation containing a -ammo-3- substituted-butanσic ac d derivative in the dosage form of tablets, powders, granules or capsules.
Also, the invention relates to a process for the preparation of a stabilized pharmaceutical preparation containing a 4-amino-3-substιtuted-butanoic acid derivative which comprises combining the 4-aιmno-3-substιtuted-butanoιc ac d derivative with an ammo acid as a stabilizer and, if necessary, an auxiliary agent necessary for manufacturing a pharmaceutical preparation.
And further, the invention relates to a process for the preparation of a stabilized pharmaceutical preparation containing a 4-ammo-3-substιtuted-butanoιc acid derivative which is in a solid or liquid form. The pharmaceutical preparation containing a 4- ammo-3-substιtuted-butanoιc acid derivative stabilized by an ammo acid according to the invention nay be formulated into various dosage forms including liquid pharmaceutical preparations such as syrups or liquid preparations or solid pharmaceutical preparations such as powders, granules, capsules or tablets .
Although the mechanism of action to stabilize a 4- amιιιo-3-s-ir)Stιtuted-butanoιc acid derivative with an amino acid has not yet been elucidated completely, it may be inferred that the ammo group of the neutral ammo acid and the carboxyl group of the neutral am o ac d would act as blocking groups on the carboxyl group of the 4-ammo-3- substituted-butanoic ac d derivative ana the ammo group of the 4-ammo-3-suo5ittuted butanoic acid derivative, respectively, to prevent autocondensation between the carboxyl group and ammo group m the molecule of the 4- amiπo-3-substιtuted-butanoic acid derivative, whereby Stabilization of the 4-ammo-3-substltutεd-butanoιc acid derivative will be eventually accomplished. However, the mechanism of action as depicted above is Dased upon a mere inference and patentability of the present invention obviously should not be influenced by whether this inference may be right or wrong.
As discussed above, the assumed mechanism of action to stabilize a 4-amino-3-substituted-butanoic acid derivative with an amino acid is based upon the so-called "ion pair" theory that the carboxyl and amino groups commonly contained in an amino acid may form the corresponding ion pairs with the amino and carboxyl groups of the 4-amino-3-5Ubstituted-butanoic aciα derivative, respectively. However, the present stabilization effect can not necessarily be accomplished by all sorts of amino acids.
More speci ically, the aminocarboxylic acid having an amino group at any position other than the α-position thereof such as the β-positiσn thereof, for example, β- alanine or, even of the α-amino acids, the amino acids having a pyrrolidine ring such as proline, hydroxyproline, etc. may show a weak stabilizing effect, while the γ-amino acids having an amino group at the γ-position thereof such as γ-aminobutyric acid show no stabilizing effect.
Accordingly, the nmino acid which may be employed as an effective stabilizer ip the present invention is restricted to the α-amino acid having one free carboxyl group and one free amino group at the α-pσsition thereof. In other words, all α-amino acids that have the said chemical structure can be used as a stabilizer in the present invention. The α-ammo acid the present invention (also referred to as an α-monoammo-monocarboxylic acid) may be any of acidic α-ammo acids, basic α-amino acids, neutral α-amino acids and adducts of acidic α-amino acids with basic α-ammo acids.
Examples of the α-amino acid which may be employed m this invention are illustrated below, but it is to be noted that the present invention should not be limited thereto.
The neutral α-amino acids may include glycme, phenylglycme, hydroxyphenylglycme, dihydroxyphenylglycine, L-alanine, hydroxy-L-alamne, -leucine, hydroxy- -leucme, dihydroxy-L-leucme, L-norleucme, methylene-L-norleucine, L-ketonorleucme, -isoleucine, hydroxy-L-isoleucine, dihydroxy-L-isoleucme, L-valine, hydroxy-L-valine, L- iεovaline, L-norvalme, hyc$roxy- -norvalιne, hydroxy- - ketonorvaline, L-methionine^ L-homomethionme, L-ethionine, -threonme, acetyl-L-threon e, L-tryptophan, hydroxy-L- tryptophan, methyl- -tryptophan, L-tyrσsme, hydroxy-lι- tyrosine, methyl-L-tyrosine, brσmo-L-tyrosine, dibromo-L- tyros e, 3, 5-diισdo-L-tyrosιne, acetyl-L-tyrosme, chloro- L-tyro5ine, L-m-tyrosme, L-levodopa, L-methyldopa, L- thyroxine, L-serine, acetyl-L-serine, L-homoserine, acetyl- -homoserine, ethyl-L-homoserine, propyl-L-homoserine, butyl-L-homoserme, L-cystine, L-ho ocystine, methyl-L- cystein, allyl-L-cysteine, propyl-L-cysteine, L- phenylalanine, dihydro- -phenylalanine, hydroxymethyl-L- phenylalanine, L-aminobutyric acid, L-aminoisobutyri acid, L-ketoaminobutyric acid, d.ιchloro-L-aminobutyric acid, dihydroxy-L-aminobutyric acid, phenyl-L-ammobutyric acid, L-aminovaleric acid, L-a inohydroxyvaleric acid, dihydrσxy- L-aminovaleric acid, L—aminoisovaleric acid, L-aminσhexanoi c acid, methyl-L-aminohexanoi' acid, L-aminoheptanoic acid, L- a inooctanoic acid and citrulline and the D- and DL-forms thereof .
The acidic α-amino acids may include I.-aspartic acid, L-glutamic acid, L-carbocysteine, L-aminσgiutaric acid, L-aminosuccinic acid, L-aminoadiplc acid, L- aminopi elic acid, hydroxy-L-aminopimelic acid, methyl-L- aspartic acid# hydroκy-L-aspartic acid, methyl-L-glutamic acid, jsαethylhydroxy-L-glutamic acid, L-methyleneglutamic acid, hydroxy-L-glutamic acicj» dihydroxy-L-glutamic acid, hydroxy-L-aminoadipic acid βr the like and the D- and DL- forms thereof. The basic α-ammo acids may include L-argmine, L- lys e, L-ornithme, L-canavanine, L-canalme, hydroxy-L- lysine, L-homoargmme, hydroxy-L-homoargmine, hydroxy-L- ornith e, L-diammopropionic acid, L-diammohexanoic acid, L-diaminobutyric acid, L-diammovaleric acid, L- diaminoheptanoic acid, L-di iiαinooctanoic ?cιd or the like and the D- and DL-forms thereof.
The αf ω-dismmodicarboxylic acid may include diam osuccm c acid, diammoglutaπc ac d, diammoadipic acid, diammopimelic acid or the like. here the acidic α-amino acid is used as a stabilizer for a 4-amino-3-_subst tuted-butanoιc acid derivative in this invention, the ammo acid may be used in the form of an alkali salt thereof such as aspartic acid Na salt, aspartic acid K salt, glutamic acid Na salt, glutamic ac d K salt, aminopimelic acid Na salt, aminopimelic acid K salt or the like; an acid amide thereof such as asparagine, hydroxyasparagine, glutamine, hydroxyglutam e, metbylβneglutamine or the like; an alkyl-substituted derivative of said acid amide such as methylasparagme, methylglutamine, ethylasparagme, ethylglutamine, isopropyiglutamine, hydroxyphenyl sparagine, hydrσxyphenylglutamine, hyUroxyethylasparagine, hydroxyethylglutamine or the like,- an alkyl ester thereof such as methyl, ethyl or propyl ester of aspartic acid, methyl, ethyl or propyl ester of glutamic acid or the like. Where the basic α-amino acid is used as a stabilizer in the invention, the amino acid may be used in the form of an acid addition salt thereof such as arginine hydrochloride, arginine acetate, lysine hydrochloride, lysine acetate, o nithine acetate or the like or a monoacylated derivative thereof such as acetyllysme, acetylornithme, acetylamino-aminobutyric acid, acetylamino- aminopropionic acid or the like.
And further, the acidic α-amino acid and the basic α-amino acid may be used in the form of the corresponding acidic amino acid-basic amino acid adduct such as aspartic acid arginine, aspartic acid lysine, aspartic acid ornithine, glutamic acid arginine, glutamic acid lysine, or glutamic acid • ornithine adduct or the like.
Any of the α-amino acid mentioned above may be used alone or in combination with two or more thereof for liquid or solid pharmaceutical preparations of a 4-amino-3- ρubstituted-butanoic acid derivative.
In preparing the liquid pharmaceutical preparation, the amino acid stabilizer of the invention may be blended with a 4-amino-3-substituted-butanoic acid derivative and then the resulting mixture may be simply dissolved in water to accomplish the object of stabilizing the 4-amino-3- substituted-butanσic acid derivative; provided that the 4- amino-3-substituted-butanoic acid derivative to be used is limited solely to the mσnoamino-monocarboxylic acid.
In preparing the liquid pharmaceutical preparation for oral administration, there may be incorporated, if required, a sweetening agent and/or a flavoring agent, which do not influence on the effect of the amino acid stabilizer. Also, the amino acids may exert the effect as a stabilizer on injections or transfusions for which sterilization such as high pressure steam sterilization is required.
When a masking effect against a bitter taste peculiar to a 4-amino-3-substituted-butanoic acid derivative is rather expected in a liquid pharmaceutical preparation, in addition to the stabilising effect, it is preferable to use glycine, -alanine, D- lanine, DL-alanine, Na glutamate and Na aspartate alone or in any combination thereof, because these amino acids have a potent buffering action on the 4-amino-3-substituted-butanoic acid derivative .
On the other hand, there are various embodiments for adding the amino acid stabilizer to a 4-amino-3- substituted-butanoic acid derivative in a solid pharmaceutical preparation. These embodiments may generally be divided into two types, i.e., a wet admixture wherein a solution of the amino acid dissolved in a solvent such as water or the like is added to the 4-amino-3-substituted- butanoic acid derivative and a dry admixture wherein the amino acid in a dry state is added to the 4-amino-3- substituted-butanoic acid derivative.
The wet admixture of the amino acid may be carried out during the manufacture of a pharmaceutical preparation of a 4-amino-3-substituted-butanoic acid derivative, for example, in a wet granulation step wherein the amino acid in the form of its solution or suspension is added to bulk powders of the 4-amino-3-5Ubstιtuted-butanoic acid derivative together with a binder and an auxiliary agent for manufacturing a pharmaceutical preparation, or in a coating Step to apply a coating to granules or tablets for the purpose of masking a bittef tast wherein the amino acid is dissolved or suspended in _} coating film base. The wet granulation step of a 4-amino-3-' substituted-butanoic acid derivative may be carried out by adopting any granulation method well-known per __ι, for example, a fiuidized granulation method, a high speed stirring granulation method, a melting granulation method or the like. There may be preferably employed a fluidized granulation method in which bulk powders of the 4-amino-3- substituted-butanoic acid derivative are fluidized and then a solution or suspension of a stabilizer and, if necessary, a binder and other auxiliary agents for manufacturing a pharmaceutical preparation may be sprayed on the fluidized powders .
In the granulation step, granulation may be carried out by adding to bulk powders of a 4-amino-3- substituted-butanoic acid derivative the stabilizer solution as described above and, if necessary, a binder such as corn starch, a cellulose derivative (e.g., hydroxypropyl- cellulose) , pσlyvinyl alcohol, a polyvinyl pyrrolidone (e.g., Kollidon-K30 or Kollidon-K25) , a copolyvidone (e.g., Kollidon-VA64) and the like in the form of a solution or suspension thereof. The stabilizer may be added to bulk powders of the 4-amino-3-substituted-butanoιc a-cid derivative by a wet or dry admixture up}.ng a bindr or other auxiliary agents for manufacturing a pharmaceutical preparation, and thereafter the granulation may be carried out. In this granulation step, there may be also incorporated, if necessary, a 'sweetening agent such as mannitσl, xylitol. sorbitol, aspartame and the like.
In the wet coating step of granules or tablets, there may be used as a film-forming material a polymeric base the form of a solution or suspension such as a cellulose derivative, e.g., hydroxypropylcellulose or hydroxypropylmethylcellulose, a polyvinyl yrrolidone, a copolyvidone, Eudragits and the like and, if necessary, a sweetening agent such as mannitol, xylitol, sorbitol, aspartame or the like. In this step, when t is rather expected to achieve a masking effect against a bitter taste of gabapentm, apart from the stabilizing effect, it is preferred, as is in the case of a liquid pharmaceutical preparation, to use L-alanme, D-alanine, DL-alanine, sodium glutamate or sodium aspartate alone or in any combination thereof. Also, when a lubricant effect is expected, it is preferable to use L-leucine, L-isoleucine, -valine, D- leucine, D-isoleucme, D-valine, DL-lsucma, DL-isoleucine or DL-valine.
Sur ce-coating of granules or tablets may be carried out by a well-known method using a fluidized bed or a rotary pan.
The dry admixture of the ammo acid may be carried out, beside the dry admixture in the aforementioned wet granulation step, a mixing step of powders prepared, for example, for compression using a tablet machine, for filling into hard capsules using a capsule filling machine or for filling using a distribution machine or the like. When a lubircant effect is expected in addition to the stabilizing effect in the above steps, t is preferable to use L-leucme, L-isoleucme, L-valme, D-leuciπe, D- isσleucme, D-valme, DL-leucme, DL-isoleucme or DL-valme. And further, 3 n tne dry ix: ng step, the ammo acid may be usually blended with, as required, an auxiliary agent for manufacturing a pharmaceutical preparation, for example, a binder or a disintegrator such as a cellulose derivative, e.g., hydroxypropylcellulose, crystalline cellulose, corn starch, partially gelatinized starch or lactose or the like and/or Λ sweetening agent such as mannitol, xylitol, sorbitol, aspartame or the like by means of a suitable mixer such as a well-known dry mixer, e.g., a V-blender or the like.
The solid pharmaceutical preparation of a 4- mιno- 3-3ubstituted-kutanoιc aciή derivative which has been stabilized by the addition of the ammo acid can be formulated the compressed dosage form of, for example, tablets or the fluidized dosage form of, for example, - 53
granules, so that the resulting dosage form may be easily ingested when orally administered to human.
Also, when the solid pharmaceutical preparation is administered in the form of an aqueous solution or suspension thereof, for example, the case of dry syrups or effervescent tablets as dissolved or suspended m water, a stabilizing effect may be accomplished as in the case of the liquid pharmaceutical preparation.
As explained above, the pharmaceutical preparation of a 4-am no-3-substιtuted-butanoic acid derivative of the invention includes both of liquid and solid pharmaceutical preparations and a total amount of the ammo acid as a stabilizer in a liquid pharmaceutical preparation may be in the range of 0.005 - 80 moles, preferably 0.01 - 70 moles, per 1 mole of the 4-amιno-3-substιtuted-butanoιc acj d derivative, and in a solid pharmaceutical preparation, it may be in the range of 0.001 - 80 moles. Although the latter case, the amino acid may preferably be used the amount as defined above, the amount may vary depending upon the dosage form, a sort of the auxiliary agent to be used as well as the amount thereof to be blended. The amino ac d when used beyond the upper limit would not noticeably lower or vitiate its effect. Thus, for example, when the ammo acid is to be blended as an auxiliary agent including triturated powders for manufacturing a pharmaceutical preparation, the upper limit of the amount to be blended is not limited to the application range as defined above. As stated above, a remarkable stabilization effect can be obtained in the present pharmaceutical preparation of a 4-amino-3-substituted-butanoic acid derivative by using the amino acid as a stabilizer. Moreover, in the case where the said preparation is in the form of a solid pharmaceutical preparation, there may be conco itantly used the humectant which is used as a stabilizer for the pharmaceutical preparation of a 4-amino-3-substituted- butanoic acid derivative as disclosed and claimed in our copending application filed on the same date, depending upon the dosage form and manufacturing steps for the prepration, whereupon the amino acid and humectant as used are not adversely prevented each other from exerting their effect as a stabilizer.
The invention win be more fully explained by way of the following examples, but it should not be construed that these examples are limiting the scope of the invention.
Example 1 In this Example, the following Samples (a) , (b) and (c) of aqueous solutions of gabapentin were tested for stability.
Preparation of samples: 1) Sample (a) was prepared by dissolving 500 mg of gabapentin crystals in water to make up a total volume of 10 ml.
2) Sample (b) was prepared by dissolving 500 mg of gabapentin crystals and 329 mg of glycine water to make up a total volume of 10 ml.
3) Sample (c) was prepared by dissolving 500 mg of gabapentin crystals and 513 mg of L-valine in water to make up a total volume of 10 ml.
Samples (a), (b) and (c) prepared as described above were stored under the conditions as defined in the following Table 3 and then a lactam content formed m each of the aqueous solutions was determined by means of HPLC. The lactam content in this example and examples hereinafter is expressed in te m of % by weight based on gabapentin. Tab! P. 3
Storage conditions Samples
(a) (b) (c) when initiated 0.005 0.005 0.005 45°C/1 week (sealed) 0.255 0.112 0.107 45°C/2 weeks (sealed) 0.528 0.220 0.227 45°C/3 weeks (sealed) 0.774 0.313 0.324 45'""C/4 weeks (sealed) 1.098 0.452 0.441
The above table shows that gabapentin in its aqueous solution could be prevented from the degradation with lapse of time (the lactam formation) by the addition of glycine or L-valine.
Example 2 In this Example, the following Samples (d) , (e) and (f) of aqueous solutions of gabapentin were tested for stability.
Preparation of samples:
1) Sample (d) was prepared by dissolving 500 mg of gabapentin crystals in ate to make up a total volume of 10 pil. 2) Sample (e) was prepared by dissolving 500 mg of gabapentin crystals and 1.5 g of xylitol in water to make up a total volume of 10 ml.
3) Sample (f) was prepared by dissolving 500 mg of gabapentin crystals, 219 mg of glycine and 1.5 g of xylitol in water to make up a total volume of 10 ml.
Samples (d) , (e) and (f) prepared as described above were stored under the conditions as defined in the following Table 4 and then a lactam content formed in each of the aqueous solutions was determined by means of HPLC.
Table 4
Storage conditions Samples
(d) (e) (f) When initiated 0.008 0.008 0.008
4S'-'c/l week (sealed) 0.253 0.311 0.178
45"C/2 weeks (sealed) 0.543 0.616 0.375
45C/3 weeks (sealed) p.846 0.947 0.570
The above table shows that gabapentin in its aqueous solution could be similarly prevented from the degradation with lapse of time (the lactam formation) by the addition of glycine even in the presence of xylitol.
Example 3 In this Example, the following Samples (g) and (h) of aqueous solutions of gabapentin were tested for stability. Preparation of samples:
1) Sample (g) was prepared by dissolving 10 g of gabapentin crystals in water to make up a total volume of 200 ml.
2) Sample (h) was prepared by dissolving 25 g of gabapentin crystals, 8.25 g of glycine, 9.75 g of DL- alanine, 100 g of xylitol and 0.05 g of perfume in water to make up a total volume of 500 ml.
Samples (g) and (h) prepared as described above were stored under the conditions as defined in the following Table 5 and then a lactam content formed in each of the aqueous solutions was determined by means of HPLC.
XaJbJj 5
Storage conditions Sampl es
(d) tf)
When initiated 0.005 " 0.004 40βC/2 weeks (sealed) 0.347 0.147 40βC/4 weeks (sealed) 0,621 0.303 40°C/6 weeks (sealed) 0.922 0.449 30°C/2 months (sealed) 0.384 0.159 30°C/4 months (sealed) 0.665 0.325 30°C/6 months (sealed) 0. .973 0. .441 25°C/6 months (sealed) 0. .341 0. .163 25°C/12 months (sealed) 0. .702 0. .310 l5°C/6 months (sealed) 0. .094 o. .039 15°C/12 months (sealed) 0, .180 0, .073 5°C/6 months (sealed) 0, .018 0, .009 5°C/12 months (sealed) 0 .033 0 .014
The above table shows that gabapentin in its aqueous solution could be similarly prevented from the degradation with lapse of time (the lactam formation) at all test temperatures by the addition of glycine and DL-alanine in the presence of xylitol and perfume. Example 4
This Example will illustrate the preparation of a Stabilized solid pharmaceutical preparation of gabapentin by the addition of the present stabilizer to gabapentin according to the wet admixture. Preparation of samples:
In this Example, pe ples (i) and (j) of gabapentin granules were prepared as follows: 1) Using a fluidized bad granulation apparatus, 72 g of water was sprayed onto 250 g of gabapentin crystals and successively a solution prepared by dissolving 5 g of hydroxypropylcellulose in 56 g of water was sprayed thereon and the product was dried to form Sample (i) of gabapentin granules.
2) Using a fluidized bed granulation apparatus, a solution prepared by dissolving 10 g of glycine in 62 g of water was sprayed onto 250 g of gabapentin crystals and successively a solution prepared by dissolving 5 g of hydroxypropylcellulose in 58 g of water was sprayed thereon and the product was dried to form Sample (j) of gabapentin granules .
Samples (i) and (i) prepared as described above were stored under the conditions as defined in the following Table 6 and than a lactam ccntent formed in each sample was determined by means of HPLC
T»hTe 6 Storage conditions Samples
(i) (j) when initiated 0.004 0.004
60°C/1 week (sealed) 0.131 0.079
60°C/2 weeks (sealed) 0.214 0.134 The above table shows that the degradation with lapse of time (the lactam formation) due to the presence of water and the binder hydroxypropylcellulose could be prevented by the presence of glycine . Example 5
This Example will illustrate the preparation of a stabilized solid pharmaceutiral preparation of gabapentin by the addition of the ammo acid to gabapentin according to the dry admixture. Preparation of samples:
In this Example, Sample (k) of gabapentin granules and Samples (1) , (m) and (n) of gabapentin tablets were prepared as follows:
1) Using a fluidized bed granulation apparatus, a solution prepared by dissolving 5 g of copolyvidoπe
(Kollιdon-VA64) and 5 g of propylene glycol in 90 g of water was sprayed onto 250 g of gabapentin crystals, which was then dried to form Sample (k) of gabapentin granules.
2) Using a rotary tablet p»achιne, the gabapentin granules prepared as described abovg were compressed to form tablets, each having a weight of 20Θ mg, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 2 - 3 kg, which were used as Sample (1) . 3) The gabapentin granules prepared as described in the above 1) were admixed with magnesium stearate at 0.4% by weight relative to the granules and then compressed using a rotary tablet machine to form tablets, each having a weight of 208 mg, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 4 - 5 kg, which were used as Sample (m) .
4) The gabapentin granules prepared as described the above 1) were admixed with L-isoleucine at 2?, by weight relative to the granules and then compressed using a rotary tablet machine to form tablets, each having a weight of 208 rag, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 4 - 5 kg, which were used as Sample (n) .
Samples (k) - (n) prepared as described above were stored under the conditions as defined in the following Table 7 and then a lactam content formed in each sample was determined by means of HPLC,
_ b.le -7 Storage conditions Samples (k) (1) (m) (n)
When initiated 0,005 0.005 0.005 0.005
60°C/1 week (sealed) 0.031 0.085 0.236 0.083
60°C/2 weeks (sealed) 0.048 0.145 0.449 0.157 It can be seen from comparison between the data of Samples (k) and (1) that the degradation with lapse of time (the lactam formation) of gabapentin could be accelerated by the compactness given by compressing wet granulates of gabapentin, while comparison between the data of Samples (m) and (n) reveals that the anticipated degradation with lapse of time (the lactam formation) of gabapentin by compacting the wet granulates could be prevented by using as a lubricant essential for compressing gabapentin L-isoleucine having a lubricant effect, instead of magnesium stearate.
Example 6 This Example will illustrate the preparation of a stabilized solid pharmaceutical preparation of gabapentin by the addition of the amino acid to gabapentin according to the dry admixture.
Preparation of samples:
In this Example, Samples (o) , (p) and (q) of gabapentin tablets were prepared as follows:
1) Using a fluidized bed granulation apparatus, a solution prepared by dissolving 5 g of lactose in 91 g of water was sprayed onto 250 g of gabapentin crystals, which was then dried to form gabapentin granules. 2) Using a rotary tablet machine, the gabapentin granules prepared as described in the above 1) were admixed with magnesium 3tearate at 0.4% by weight relative to the gabapentin granules and then compressed to form tablets, each having a weight of 208 mg, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 3 - 4 kg, which were used as Sample (o) .
3) The gabapentin granules prepared as described in the above 1) were admixed with calcium stearate at 0.2% by weight relative to the granules and then compressed using a rotary tablet machine to form tablets, each having a weight of 208 mg, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 3 - 4 kg, which were used as Sample (p) .
4) The gabapentin granules prepared as described in the above 1) were admixed with L-isoleucine at 2 ?> by weight relative to the granules and then compressed using a rotary tablet machine to form tablets, each having a weight of 212 mg, a diameter of 8 mm, a thickness of 4.3 mm and a hardness of 3 - 4 kg, which were used as Sample (q)~ . Samples (o) - (ςj) prepared as described above were stored under the condition_| as defined in the following Table 8 and then a lactam content formed in each of the samples was determined by means of HPLC. lable S
Storage conditions Samples
(o) (p) (q)
When initiated 0.005 0.005 0.005
60°C/1 week (sealed) 0.236 0.118 0.068
60°C/2 weeks ( sealed) 15.625 0.267 0.150
50°C/ 85% humidity/ 2 weeks ( sealed) 0.187 0.090 0.082
50°C/ 85% humidity/ 4 weeks ( sealed) 10.259 0.440 0.378
It can be seen from the table that the anticipated degradation with lapse of time (the lactam formation) of gabapentin by compacting the wet granulates could be prevented by using as a lubricant essential for compressing gabapentin L-isoleucine having a lubricant effect, instead of magnesium stearate or calcium stearate.
Example 7
This Example will illustrate that gabapentin could be stabilized by the addition of the amino acid according to the dry admixture. Preparation of samples: 1) From 600 mg of gabapentin crystals was prepared by means of a mortar a powdery sample in a compacted state as Sample (r) .
2) From 600 mg of gabapentin crystals together with 180 mg of glycine was prepared by means of a mortar a powdery sample in a compacted state as Sample (s) .
Samples (r) and ' * ) prepared as described above were stored under the conditions as defined m the following Table 9 and then a lactam content formed in each of the samples was determined by means of HPLC.
Table 9 Storage conditions Samples
(r) (s) When initiated 0.008 0.008
60"C/2 weeks (sealed) 0.136 0.130
60°C/3 months (sealed) 14.326 0.926 50"C/85% humidity/2 weeks (open) 0.012 0.013 50°C/85% humidity/3 months (open) 0.013 0.016
It can be seen frpm the above table that the anticipated degradation with lapse of time (the lactam formation) of gabapentin in a compacted state could be prevented by the addition cf the am o acid according to the dry admixture.
Example B In this Example, the following samples (t) , (u) and (v) were tested for stability in aqueous solutions of pregabalin.
Preparation of samples:
1) Sample (t) wε prej..red _.*/ dissolving 1 g of pregabalin crystals in water to make up a total volume of 50 ml.
2) Sample (u) was prepared by dissolving 1 g of pregabalin crystals and 0.94 g of glycine in water to make up a total volume of 50 ml.
3) Sample (v) was prepared by dissolving 1 g σf pregabalin crystals and 1.47 g σf L-valine in water to make up a total volume of 50 ml . Samples (t) , !u) md (v) prepared as described above were stored under the conditions as defined, in the following Table 10 and then a content of the dehydrated condensate formed in each αf the aqueous solutions was determined by means of HPLC. In this Example and the following Examples, a content of the dehydrated condensate formed is expressed in terms of % by weight, based on pregabalin. Table 10
Storage conditions Samples
(t) (u) (v)
When initiated <0.001 <0.001 <0 .001 45°C/1 week (sealed) 0.049 0.024 0. 024 45°C/4 weeks (sealed) 0.099 0.051 0. 050 45°C/6 weeks (sealed) 0.159 0.079 0. ,077
The above table shows that pregabalin its aqueous solution could be prevented from the degradation with lapse of time (the condensation with dehydration) by the addition σf glycine or L-valine-
Example 9
This Example will illustrate the preparation of a stabilized solid pharmaceutical preparation of pregabalin by the addition of the amino acid to pregabalin according to the dry admixture. Preparation of samples:
In this Example, Sample (aa) of pregabalin granules and Samples (ab) , i^c) and (ad) of pregabalin tablets were prepared as follo s: Preparation of samples: 1) 1 g of pregabalin crystals was prepared to powdery Sample (aa) m a compacted state by means of a mortar.
2) 1 g of pregabalin crystals was blended with 10 mg of magnesium stearate by means of a mortar to prepare mixed powdery Sample (ab) m a compacted state.
3) 1 g of pregabalin crystals was blended with 30 mg of talc by means of a mortar to prepare mixed powdery Sample (ac) in a compacted state.
4) 1 g of pregabalin crystals was blended with 30 mg of L-leucine by means of a mortar to prepare mixed powdery
Sample (ad) a compacted state.
Samples (aa) , (ab) , (ac) and (ad) prepared as described above and untreated pregabalin crystals were stored under the conditions as defined in the following Table 11 and then a content o the dehydrated condensate formed in each σf the samples was determined by means of HPLC.
Table 11 Storage conditions Untreated Samples pregabalin (aa) (ab) (ac) (ad)
When initiated <0.00J <0.001 <0.001 <0.001 <0.001
80°C/1 week (sealed) 0.006 0.030 0.092 0.035 0.022
60°C/2 weeks (sealed) 0.001 0.041 0.056 0.051 0.033 The above table shows that pregabalin could be prevented from the degradation with lapse cf time (the condensation with dehydration) by the use cf an amino acid as a lubricant which is considered as an essential material for manufacturing a solid pharmaceutical preparation.
Example 10 In this Example, the following Samples (ae) and (af) were tested for stability in aqueous solutions of baclofen. Preparation of samples:
1) Sample (ae) was prepared by dissolving 0.05 g of baclofen crystals in water to make up a total volume σf 50 ml
2) Sample (af) was prepared by dissolving 0.0b g of baclofen crystals and 0.05 g of glycine in water to make up a total volume of 50 ml.
Samples (ae) and (af) prepared as described above were stored under the conditions as defined in the following Table 12 and then a content of the dehydrated condensate formed in each of the aqueous solutions was determined by means of HPLC,
In this Example and the following Example, a content of the dehydrated condensate thus formed is expressed in terms of % by weight, based en baclofen. - 73
Table 12
Storage conditions Samples
(ae) (af )
When initiated 0.10 0.10 60°c/l week (sealed) 0.53 0.28 60°c/2 weeks (sealed) 0.92 0.54 60°C/3 weeks (sealed) 1.33 0.80 4b"C/2 weeks (sealed) 0.33 0.21 45°C/Θ weeks (sealed) 0.62 0.29
121°C/15 minutes (high pressure steam sterilization) 0.31 0.21
The above table shows that baclofen could be prevented from the degradation with lapse of time (the condensation with dehydration) in its aqueous solution by the addition of glycine under all the storage and heating conditions.
Example 11
In thig Example, the stabilization of baclofen according to the wet admixture with the amino acid was tested for the following SampJ.es (ag) and (ah) of baclofen. Preparation o samples: 1) Sample (ag) as prepared by wetting 200 mg of baclofen crystals with 0.1 ml of water, forming granular powders by means of a mortar and then drying.
2) Sample (ah) was prepared by wetting 200 mg of baclofen crystals with 0.1 ml of a 2% aqueous solution of L- isoleuc e, forming granular powders by means σf a mortar and then drying.
Samples (ag) and (ah) prepared as described above and untreated baclofen crystals were stored under the conditions as defined in the following Table 13 and then a content of the dehydrated condensate formed in each of the samples was determined by means of HPLC.
Table 13 Storage conditions Untreated Samples baclofen (ag) (ah)
When initiated Q . 10 0 . 08 0 . 07
60UC/1 week ( sealed) 0 , 36 0 . 67 0 .28
60°C/2 weeks (sealed) 0,57 1.05 0.30 60°C/3 weeks (sealed) (J.JO 1.33 0.32
The above table shows that the degradation of baclofen with lapse oi time (the condensation with dehydration) could be accelerated by the granulation using 9/59573
- 75 -
water and could be prevented by wet admixture of L-leucme.
According to the present invention, the stabilization of a pharmaceutical preparation containing a 4-ammo-3-substιtuted-butanoιc acid derivative can be accomplished by the additicn of an am o acid. Moreover, the stabilization by the addition of an am o acid can be accomplished not only in solid pharmaceutical preparations but also in liquid pharmaceutical preparations, stabilization of which has not been succeeded. Thus, he present invention can provide diverse means to administer a pharmaceutical preparation of a 4-ammo-3-tsubstιtuted- butanoic acid derivative; for example, he 'difficulty encountered in the prior art when admmιst|ered to children may be avoided by forming a pharmaceutical preparation of gabapentin the dosage form of a liquid pharmaceutical preparation, and others. The present invention can be expected to greatly contribute to the development of a stabilized pharmaceutical preparation of a 4-ammo-3- substituted-butanoic acid deriva e.

Claims

What is claimed is:
1. A stabilized pharmaceutical preparation containing a 4-amino-3-substιtuted-butanoιc acid derivative which comprises a 4-ammo-3-substιtuted-butanoιc acid derivative having the general formula
NH,CH7-C-CH,C00H R-_ Rz wherein,
Ki is a hydrogen atom, a hydroxyl group, a methyl group or an ethyl group;
Rj is a onovalent group selected from" a straight or branched alkyl group of 3 - 8 carbon atoms ; a straight or branched alkyl ne group of 3-8 carbon atoms; a straight or branched alkyl group of 3 - 8 carbon atoms which is mono- or di-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkyl group of 3 - 8 carbon atoms; a cycloalkyl group of 3 - 8 carbon atoms which is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed rmg group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 4 - 6 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 4 - 8 carbon atoms wherein said phenyl ring is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; a condensed rmg group formed by ortho-fusion □£ a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring w th a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms wherein said phenyl ring is mono-, di- or tri-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an ammo group, a nitro group, a carboxyl group or a carboalkoxy group; an alkylcycloalkyl group wherein said cycloalkyl has 3 - 8 carbon atoms and is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O-, -s- or -SS-; an alkylcycloalkyl group wherein said cycloaJ yl has 3 - 8 carbon atoms, is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O- , -S- or -SS- and is mono-, di- or tπ-substituted w th a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH.,-) is replaced by -0-, -NH-, -£»-, -50- or -S(O),-; a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH,-) is replaced by -O-, -NH-, -S-, -SO- or -3(0)2-, and one or two of the unsubstituted methylene groups (-CH.,-) are mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an ammo group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH,-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, =N-, -S-, -SO- or -S (0)^,-; a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one σf the methylene groups (-CH-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, =N-, -S-, -SO- or -S(0),-, and one or two of the unsubstituted methylene groups (-CH-) being rconσ- or di-substituted with a halogen atom, a trifl oromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed rinq group formed by ortho-fusion of a pheny) rmg with a cycloalkyl group of 5 - fl carbon atoms wherein one of the methylene groups (-CH,-) is replaced by -O-, -NH-, -5-, -SO- or -S (O) ,- ; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group σf 5 - 8 carbon atoms wherein one of the methylene groups (-CH2-) is replaced by -0-, -NH-, -S-, -SO- or -S(O),-, said phenyl group being mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of b - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH..-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, =N-, -S-, -50- or -S (0) ,-; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH,-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, -N-, -S-, -SO- or -5(0)2-, said phenyl ring being mono- or di-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl 'jroup, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; an alkylcycloalkyl group wherein said cycloalkyl has 5 - 8 carbon atoms and s linked to an alkylene group having
1 - 4 carbon atoms optionally interrupted with -0-, -S- or
-SS-, one of the methylene groups (-CH.,-) in said cycloalkyl ring being replaced by -0-, -NH-, -S-, -SO- or -S(0),-; an alkylcycloalkyl roup wherein said cycloalkyl has 5 - 8 carbon atoms and is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O-, -S- or -5S-, and one of the methylene groups (-CH.,-) in said cycloalkyl ring being replaced by -o-, -NH-, -S-, -SO- or
-S (o) ,- and one or two of the unsubstituted methylene groups (-CH,-) being mono-, di- or tri-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, ar: alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a phenyl or naphthyl group; a phenyl group substituted with a methylenedioxy group; a phenyl or naphthyl group which is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group, a carboxyl group, a phenoxy group, a phenylmethoxy group, a phenylmethoxy group wherein said phenyl ring s mono-substituted w th a halogen atom, trifluoromethyl group, an alkoxy group, an ammo group, a nitro group, a carboxyl group or a carboalkoxy group, a cycloalkylmethoxy gvoup having 5 - 9 carbon atoms m the cycloalkyl rmg, a c cloalkenylmethoxy group having 5 - 8 carbon atoms the cyc-i-oalkenyl ring, a cycloalkanedienylmethoxy group having 5 - 8 carbon atoms m the cycloalkanedienyl ring, a cycloalkylmethoxy group wherein one of the methylene groups (-CH:-) in said cycloalkyl ring having 5 - 8 carbon atoms is replaced by -O-, -NH-, -S-, -SO- or -S(0)L-, a cycloal enylmethoxy group wherein one of the mcthyle- c groups (-CH,-) in said cycloalkenyl ring having 5 - 8 carbon atoms s replaced by -O-, -NH-, -=N-, -S-, -SO- o" -S(O)--, a cycloalkanedienylmethoxy group wherein one σf the methylene groups (-CH^,-) said cycloalkaneαiεnyi ring having 5 - 8 carbon atom3 is replaced by -O-, -NH-, =N-. »S-, -SO- or -S (O) _,- group, a cycloalkylmethoxy group havin 5 - 8 carbon atoms m the cycloalkyl ring wherein saiej cycloalkyl ring is mono-substituted with a halcgen atom, trifluoromethyl group, a hydroxy group, an alkyl group, an alkoxy group, an ammo group, a nitro group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH,-) in said cycloalkyl ring is replaced by -0-, -NH-, -S-, -SO- or -5(0),-, a cycloalkenylmethoxy group having 5 - 8 carbon atoms in the cycloalkenyl ring wherein said cycloalkenyl ring is mono-substituted with a halogen atom, a trifluoromethyl group, a hydroxy group, an alkyl group, an alkoxy group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH,-) in said cycloalkenyl ring is replaced by -O-, -Nil-, -N-, -5-, -SO- or -S(0),,-, or a cycloal kanedienylmethoxy gr. up having 5 - 8 carbon atoms in the cycloalkanedienyl ring wherein said cycloalkanedienyl ring is mono-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH,-) in said cycloalkanedienyl ring is replaced by -0-, -NH-, -N-, -S-, -SO- or -S (Q) ,-.; an alkylphenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -S- or -SS-; an alkyl-O-, -S- or -S5-phenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms via -0-, -5- or -SS-; an -0-, -S- or -SS-phenyl group; a diphenylamino group: an alkylphenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -S- or -SS- and mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, a alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; an alkyl-O-, -S- or -SS-phenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms via -0-, -S- or -SS- and mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; an -0-, -S- or -SS-phenyl group wherein said phenyl group is mono-, di- or tri»aubstituted w th a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; or
Ri and R,, together with the carbon atom to which they are attached, may form a divalent group selected from: a cycloalkylidene group of 5 - 8 carbon atoms; a cycloalkylidene group of 5 - 8 carbon atoms which is mono-, di-, tri- or tetra-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, a cycloalkyl group, a phenyl group, an amino group, a nitro group or a carboxyl group; a cycloalkylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH2-) in said cycloalkyl ring is replaced by -0-, -NH-, -S-, -SO- or -S(O)..-; a cycloalkylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH,-) in said cycloalkyl ring is replaced by -0-, -NH-, -S-, -SO- or -S (O) ,- group and one or more of the unsubstituted methylene groups (-CH.,-) in said cycloalkyl ring are mono-, di-, tri- or tetra-substituted ith a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an am o group, a nitro group, an oxo group, a carboxyl group or a .carboalkoxy group; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms which is mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, a cycloalkyl group, a phenyl group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH,-) m said cycloalkenyl ring or cycloalkanedienyl ring is replaced by -0-, -NH-, --N-, -S-, -SO- or -S(O) -; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - θ carbon atoms wherein one of the methylene groups (-CH,-) in said cycloalkenyl ring or cycloalkanedienyl ring j.β replaced by -0-, -NH-, -N-, -S-, -SO- or -5(0).- group and oj>e or more of the unsubstituted methylene groups (-CH,-) iη paid cycloalkenyl ring or cycloalkanedienyl ring are mono-, di-, tri- or tetra-substituted wi h a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an ammo group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring group Tor ed by ortho-fusion σf a phenyl r ng with a cycloalkylidene group of 4 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl rmg with cycloalkylidene group of 4 - 8 carbon atoms, sa^d phenyl ring being mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an am o group, a nitro group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl r ng with a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of b - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenylidene group of b - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms, said phenyl ring being mono- or di-substitυted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an ammo group, a nitro group, a carboxyl group or a carboalkoxy group; an Of-ammo acid; and, if necessary, an auxiliary agent for manufacturing a pharmaceutical preparation.
2. The stabilized pharmaceutical preparation containing the 4-ammo-3-substituted-butanoιc acid derivative as claimed in claim 1 wherein said ot-amino acid is one or more selected fro.v the L-, D- and DL-formo of neutral α-amino acids; alkali salts, acid amides, alkyl-substituted derivatives of acid amides or alkyl esters of the L-, D- and DL-forms of acidic α-ammo acids; acid addition salts or onoacylated derivatives of the L-, D- and DL-forms of basic α-anino acids; α, ω-dιammodιcarbθ"<ylic acids; and acidic amino acid-basic amino acid adducts of the L-, D- and DL-forms of acidic -amino acids and the L-, D- and DL- forms of basic -ammo acid:*.
3. The stabilized pharmaceutical preparation containing the 4-ammo-3-s bεtituted-butanσic acid derivative as claimed in cl^im 2 wherein said α-amino acid is one or more selected from neutral α-amino acids consisting of glycine, phenylglycine, hydroxyphenylglyc e, dihydroxyphenylglycine, L-alamne, hydroxy-L-alanme, L-leucme, hydroxy-L-leucine, dihydroxy-L-leucine, L-norleucine, methylene-L-norleucine, L-ketonσrleucine, L-isoleucine, hydroxy-L-isoleucme, dihydroxy-L-isoleucine, L-valine, hydrσxy-L-valine, L- isovalme, L-norvaline, hydroxy-L-norvaline, hydroxy-L- ketonorvaline, L-methionine, L-homomethionine, -ethionine,
L-threonine, acεtyl-L-thr :onine, L-tryptσphan, hydroxy-L- tryptophan, methyl-L-trypι_cphan, L-tyrosme, hydroxy-L- tyrosine, methyl-L-tyrosme, bromo-L-tyrosine, dibromo-L- tyrosme, 3, 5-dιιodo-L-tyrosine, acetyl-L-tyrosine, chloro- L-tyrosine, L-m-tyrosine, L-levodopa, L-methyldopa, L- thyroxme, L-serine, acetyl- -sεrine, L-homoserine, acetyl- L-homo5erine, ethyl-L-homoseriπe, propyl-L-homoserine, butyl-L-homoserine, L-cystins, L-hσmocystme, methyl-L- cysteine, allyl-L-cysteine, ρropyl-L-cysteme, L- phenylalanine, dihydro-L-phenylalanine, hydroxymethγl-L- phenylalanine, L-aminobutyric acid, l.-aminoisσbutyric acid, L-ketoaminobutyric acid, dichloro-L-aminobutyπc acid, dihydroxy-L-aminobutyric acid, phenyl-L-am nobutyπc acid, H.-aminovaleric acid, L-aminohydroxyvaleric acid, dihydroxy- L-aminovaleric acid, L-aminoisovaleric acid, L-ammohexanoic acid, methyl-.i-ammσhexanoie acid, L-aminoheptanoic acid, L- aminooctanoic acid and citzulline and the D- and DL-forms thereof; acidic α-amino acids consisting of L-aspartic acid, L- gluta ic acid, L-carbocysteine, L-aminoglutaric acid, L- aminosuccmic acid, L-ammoadipic acid, L-aminopimelic acid, hydroxy-L-ammcpimelic acid, methyl-L-aspartic acid, hydroxy-L-aspartic acid, ethyl-L-glutamic acid, methyl- hydroxy-L-glutamic acid, ι,-methylcneglutamιc acid, hydroxy- L-glutamic acid, dihydroxy-L-glutamic acid and hydroxy-L- ammoadipic acid and the O- and DL-forms thereof; basic α-amino acids consisting of L-argmme, L-lysme, L-ornith e, L-canavanine, L-canaline, hydroxy-L-lysme, L- homoarginine, hydroxy-L-homoarginme, hydroxy-L-ormthme, L-d aminopropionic acid, L-diaminohexanoic acid, L- diaminobutyric acid, L-diammovaleric acid, L- diammoheptanoic acid, and L-diaminooctanoic acid and the D- and DL-forms thereof; and α,ω-dιaminodιcarboxylic acids consisting of diaminosucci ic acid, diaminoglutaric acid, diaminoadipic acid and diaminopimelic acid; provided that, when said α-amino acid is an adipic α- amino acid, it is used the form σf the corresponding alkali salt, acid amide, alkyl-substituted derivative of acid amide or alkyl ester thereof, or when said α-amino acid is a basic α-amino acid, it is used in the form of the corresponding acid addition salt or monoacylatec derivative thereof, or said acidic α-amino acid and said basic α-amino acid are also used in the form of the corresponding acidic amino acid-basic ammo acid adduct.
4. The stabilized pharmaceutical preparation containing a 4-amino-3-substituted-butanic acid derivative as claimed in any of claims 1 - 3 wherein a total amount of said α-amino acid is in the range of 0.001 - 80 moles per mole of the 4-ammo-3-substituted-butanic acid derivative.
5. The stabilized pharmaceutical preparation containing a 4-amino-3-≤ubstιtuted-butanιc acid derivative as claimed in any of claims 1 - 4 wherein t is in the form of liquid preparations.
6. The stabilized pharmaceutical preparation containing a 4-aκιino-3-substituted-bυtanic acid derivative as claimed in claim 5 wherein it is in the dosage form of liquid preparations, syrups pr injections. 7, The stabilized pharmaceutical preparation containing a 4-amino-3-subβtituted-butanic acid derivative as claimed in any of claims 1 - 4 where i . it is in the form of solid preparations.
8. The stabilized pharmaceutical preparation containing a 4-amino-3-substituted-butanic acid derivative as claimed in claim 7 wherein it is in the dosage form of tablets, powders, granules or capsules. 9. The stabilized pharmaceutical preparation containing a 4-amino-3-substituted-butanic acid derivative as claimed m any of claims 1 - 8 wherein it is a gabapentin-containing preparation, a pregabalin-containing preparation, a baclofen-containing preparation, or a preparation containing 3-aminomethyl-4-cyclohexyl-butanoic acid, 3-a inomethyl-5-cyclohexyl-pentanoic acid, 3- aminomethyl-4-phenyl-butanoic acid or 3-aminomethyl-5- phenyl-pentanoic acid. 10. A process for the preparation of a stabilized pharmaceutical preparation containing a 4-ammo-3- substituted-butanoic acid derivative having the general formula HJCHJ.-C-CHJCOOH
wherein,
Rx is a hydrogen atom, a hydroxyl group, a methyl group or an ethyl group;
R, is a mσno alent group selected from; a straight or branched alkyl group of 3 - 8 carbon atoms; a straight or branched alkylene group of 3-8 carbon atoms ; a straight or branched alkyl group of 3 - 8 carbon atoms which is mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkyl group of 3 - 8 carbon atoms; a cycloalkyl group of 3 - 8 carbon atoms which is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring i h a cycloalkyl group σf 4 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 4 - 8 carbon atoms wherein said phenyl ring is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by σrtho-fusion σf a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group σf 5 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group σf 5 - 8 carbon atoms wherein said phenyl ring is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; an alkylcycloalkyl group wherein said cycloalkyl has 3 - 8 carbon atoms and is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -5- or -5S-; an alkylcycloalkyλ group wherein said cycloalkyl has 3 - 8 carbon atoms, is linjcβd to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O-, -S- or -5S- and is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl grβup, a hydroxyl group, an alkyl group, an alkoxy . group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH2-) is replaced by -0-, -NH-, -S-, -50- or -5(0).,-; a cycloalkyl group of 5 - θ carbon atoms wherein one of the methylene groups (-CH.-) is replaced by -0-, -NH-, -S-, -SO- or -S(0) -, and one or two of the unsubstituted methylene groups (-CH^-) are mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of ' - 8 carbon atoms, one of the methylene groups (-CH,-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, -N-, -S-, -SO- or -S(0)?-; a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH.,-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, -N-, -S-, -50- or -S(0)2-, and one or two of the unsubstituted methylene groups (-CH,-) being mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring gro ip formed by ortho-fusion of a phenyl ring with a cyciσaj.' 'I group of 5 - 8 carbon atoms wherein one of the mathyl groups (-CH,-) is replaced by -0-, -NH-, -S-, -50- or -S('J) -; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkyl group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH-) is replaced by -O-, -NH-, -S-, -SO- or -S(0)2-, said phenyl group being mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio r°up, an
Figure imgf000098_0001
group, a nitro group, a carboxyl group or J carboalkoxy group; a condensed ring g oup formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH2-> in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -0-, -NH-, -N-, -S-, -SO- or -S(O),,-; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenyl group of 5 - 8 carbon atoms or a cycloalkanedienyl group of 5 - 8 carbon atoms, one of the methylene groups (-CH2-) in said cycloalkenyl ring or cycloalkanedienyl ring being replaced by -O-, -NH-, =N~, -5-, -SO- or -5(0)2-, said phenyl ring being mono- or di-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group; an alkylcycloalkyl group wherein said cycloalkyl has 5 - 8 carbon atoms and is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -S- or -SS-, one of the methylene groups (-CH2-) in said cycloalkyl ring being replaced by -O- , -NH-, -5-, -SO- or -S(0);-; an alkylcycloalkyl φroup wherein said cycloalkyl has 5 - 0 carbon atoms and is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O-, -5- or -SS-, and one σf the methylene groups (-CH-) in said cycloalkyl ring being replaced by -0-, -NH-, -S-, -SO- or
-S(0)2- and one or two of the unsubstituted methylene groups (-CHj-) being mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a phenyl or naphthyl group; a phenyl group substituted with a ethylenedioxy group; a phenyl or naphthyl group which is mono-, di- or tri-substituted with a halogen atom, a tri luoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group, a carboxyl group, a phenoxy group, a phenylmethoxy group, a phenylmethoxy group wherein said phenyl ring is mono-substituted with a halogen atom, trifluoromethyl group, an alkoxy group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group, a cycloalkylmethoxy group having 5 - 8 carbon atoms in the cycloalkyl ring, a cycloalkenylmethoxy group having 5 - B carbon atoms in the cycloalkenyl ring, a cycloalkanedienylmethoxy group having 5 - 8 carbon atoms in the cycloalkanedienyl r ng, a cycloalkylmethoxy group wherein one of the methylene groups (-CH-) in said cycloalkyl ring having 5 - β carbon atoms is replaced by -0-, -NH-, -S-, -SO- or -S(0)7-, a cycloalkenylmethoxy group wherein one of the methylene groups (-CH..-) in said cycloalkenyl ring having 5 - 8 carbon atoms is replaced by -0-, -NH-, =N-, -S-, -SO- or -5(0).,-, a cycloalkanedienyl- methoxy group wherein one of the methylene groups (-CH2-) in said cycloalkanedienyl ring having 5 - 8 carbon atoms is replaced by -0-, -NH-, -N-, -S-, -SO- or -5(0),- group, a cycloalkylmethoxy group having 5 - 8 carbon atoms in the cycloalkyl ring wherein said cycloalkyl ring is mono-substituted with a halogen atom, trifluoromethyl group, a hydroxy group, an alkyl group, an alkoxy group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH..-) in said cycloalkyl ring is replaced by -0-, -NH-, -S-, -SO- or -S(0),-, a cycloalkenylmethoxy group having 5 - 8 carbon atoms in the cycloalkenyl ring wherein said cycloalkenyl ring is mono-substituted with a halogen atom, a trifluoromethyl group, a hydroxy group, an alkyl group, an alkoxy group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH,-) in said cycloalkenyl ring is replaced by -0-, -NH-, =N-, -S-, -SO- or -SfO),,-, or a cycloalkanedienylmethoxy group having 5 - 8 carbon atoms in the cycloalkanedienyl ring wherein said cycloalkanedienyl ring is mono-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group and one of the methylene groups (-CH2-) in said cycloalkanedienyl ring is replaced by -0-, - H-, =N-, -S-, -SO- or -S(0),-; an alkylphenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -O-, -S- or -SS-; an alkyl-O-, -S- or -SS-phenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms via -O-, -S- or -SS-; an -0-, -S- or -SS-phenyl group; a diphenylamino group: an alkylphenyl. group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms optionally interrupted with -0-, -S- or -SS- and mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, a alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; an alkyl-O-, -Ξ- or -55-phenyl group wherein said phenyl group is linked to an alkylene group having 1 - 4 carbon atoms via -0-, -S- or -SS- and mono-, di- or tri-substituted' with a halogen atom, a tri luoromethyl . group, a hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; an -0-, -S- or -SS-phenyl group wherein said phenyl group is mono-, di- or tri-substituted with a halogen atom, a trifluoromethyl group, 3 hydroxyl group, an alkyl group, an alkoxy group, an amino group, a nitro group or a carboxyl group; or Rt and Rv, together with the carbon atom to which they are attached, may form a divalent group selected from: a cycloalkylidene group of 5 - 8 carbon atoms; a cycloalkylidene group of 5 - 8 carbon atoms which is mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, a cycloalkyl group, a phenyl group, an amino group, a nitro group or a carboxyl group; a cycloalkylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH-,-) in said cycloalkyl ring is replaced by -O-, -NH-, -β-, -SO- or -5(0),-; a 'cycloal ylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH2-) in Said cycloalkyl ring is replaced by -O-, -NH-, -S-, -50- or -S(O),- group and one or more of the unsubstituted. methylene groups (-CH2-) in said cycloalkyl ring are mono-, di-, tri- or tetra-substituted with a halogen atom, a trirluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, an' oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group σf 5 - 8 carbon atoms; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms which is mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, en alkylthio group, a cycloalkyl group, a phenyl group, an amino group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH,-) in said cycloalkenyl ring or cycloalkanedienyl ring iψ replaced by -O-, -NH-, =N-, -S-, -SO- or -5(0),-; a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms wherein one of the methylene groups (-CH,-) in said cycloalkenyl ring or cycloalkanedienyl ring is replaced by -O-, -NH-, =N-, -S-, -50- or -S(0)7- group and one or more of the unsubstituted methylene groups (-CH2-) in said cycloalkenyl ring or cycloalkanedienyl ring arc mono-, di-, tri- or tetra-substituted with a
Figure imgf000105_0001
atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an ammo group, a nitro group, an oxo group, a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkylidene group of 4 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkylidene group of 4 - 8 carbon atoms, said phenyl ring bsing mono-, di-, tri- or tetra-substituted with a halogen atom, a trifluoromethyl group, a hydroxyl group, an alkyl group, an alkoxy group, an alkylthio group, an amino group, a nitro group, . a carboxyl group or a carboalkoxy group; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenylidene group of 5 - 8 carbon atoms or a cycloalkar÷edien} idene group of 5 - 8 carbon atoms; a condensed ring group formed by ortho-fusion of a phenyl ring with a cycloalkenylidene group σf 5 - 8 carbon atoms or a cycloalkanedienylidene group of 5 - 8 carbon atoms, said phenyl ring bei ig mono- or di-substituted with a halogen atom, a trifluoromerhyl group, a hydroxyl group, an alkyl group, an alkoxy gro o, an alkylthio group, an amino group, a nitro group, a carboxyl group or a carboalkoxy group, which comprises conujj.ning the 4-amino-3-substituted- butanoic acid derivative with an α-amino acid and, if necessary, an auxiliary agent for manufacturing a pharmaceutical preparation.
11. The process as claimed in claim 10 wherein said ot- amino acid is one or more εelected from the -, D- and DL-forms σf neutral α-amino acids; alkali salts, acid amides, alkyl-substituted derivatives of acid amides or alkyl esters of the L-, D- and DL-forms of acidic α-amino acids; acid addition salts or monoacylated derivatives of the L-, D- and DL-forms σf basic α-amino acids; α, ω-diaminodicarboxylic acids; and acidic amino acid-basic amino acid adducts of the L-, D- and DL-forms of acidic α-amino acids and the L-, D- and DL- forms of basic' α-amino acids.
12. The process as claimed in claim 10 wherein said α- amino acid is one or more selected from neutral α-amino acids consisting σf glycine, phenylglycine, hydroxyphenylglycme, dihydroxyphenylglycine, L-alanine, hydrσxy-L-alanine, L-leucine, hydroxy-L-leucine, dihydroxy-L-leucine, L-norleucine, methylenε-L-norleucme, L-ketonorleucine, L-isoleucine, hydroxy-L-isoleucine, dihydroxy-L-isoleucine, L-valine, hydroxy-L-valine, L- isovaline, L-norvaline, hydrσxy-L-norvaline, hydroxy-L- ketonorvaline, L-methionine, L-homomethionine, L-ethionine, L-threonine, acetyl-L-threonine, L-tryptophan, hydroxy-L- tryptophan, methyl-L-tryptophan, L-tyrosine, hydroxy-L- tyrosine, methyl-L-tyrosine, bromo-L-tyrosine, dibromo-L- tyrosine, 3, 5-diiodo-L-tyrosine, acetyl-L-tyrσsine, chloro- L-tyrosine, L-m-tyrosine, L-levodopa, L-methyldopa, L- thyroxine, L-serine, acetyl-L-serine, L-hσmσserine, acetyl- li-homoserine, ethyl-L-homoserine, propyl-L-homσεerme, butyl-L-horaoserine, L-cystine, L-homocystine, methyl-L- cysteine, allyl-L-cysteinβ, propyl-L-cysteine, L- phenylalanine, dihydro-L-pfcenylalanine, hydroxymethyl-L- phenylalanine, L-aminobutyric acid, L-ammoisobutyric acid, L-ketoaminobutyric acid, dichloro-L-aminobutyric acid, dihydrσxy-L-aminobutyric acid, phenyl'-L-aminobutyric acid, L-aminovaleric acid, L-aminohydroxyvaleric acid, dihydroxy- L-aminovaleric acid, L-aminoisovaleric acid, L-aminohexanoic acid, methyl-L-aminσhexanoic acid, L-aminoheptanoic acid, L- aminooctanoic acid and citrulline and the D- and DL-forms thereof; acidic α-amino acids consisting of L-aspartic acid, L- glutamic acid, L-carbocysteine, L-aminoglutaric acid, L- aminosuccinic acid, L-aminoadipic acid, L-aminopimelic acid, hydroxy-L-aminopimelic acid/ methyl-L-aspartic acid, hydroxy-L-aspartic acid, methyl-L-glutamic acid, methyl- hydroxy-L-glutamic acid, L-methyleneglutamic acid, hydroxy- L-glutamic acid, dihydroxy-L-glutamic acid and hydroxy-L- aminoadipic acid and the D- and DL-forms thereof; basic α-amino acids consisting of L-arginine, L-lysine, L-ornithine, L-canavanine, L-canaline, hydroxy-L-lysme, L- homσarginine, hydroxy-L-homoarginine, hydroxy-L-ornithine, L-diaminopropionic acid, L-eJiaminohexanoic acid, L- diaminobutyric acid, L-diaπ»inovaleric acid, L- diaminoheptanoic acid, and -diaminooctanoic acid and the D- and DL-forms thereof; and α, ω-diaminodicarboxylic acids consisting of diaminosuccinic acid, diamihbglutaric acid, diaminoadipic acid and diami opimelic acid; provided that, when said α-amino acid is an acidic α- amino acid, it is used in the form of the corresponding alkali salt, acid amide, alkyl-substituted derivative of acid amide or alkyl ester thereof, or when said α-amino acid is a basic α-amino acid, it is used in the form of the corresponding acid addition salt or monoacylated derivative thereof, or said acidic α-amino acid and said basic α-amino acid are also used in the form of the corresponding acidic amino acid-basic amino acid adduct.
13. The process as claimed in any of claims 10 - 12 wherein the stabilized pharmaceutical preparation containing a 4-aminσ-3-substituted-but3noic acid derivative is in the form of liquid preparations. 14. The process as claimed in claim 5 wherein the liquid preparation is in the dosage form of liquid preparations, syrups or injections.
15- The process as claimed in any of claims 10 - 12 wherein the stabilized pharmaceutical preparation is in the form of solid preparation*. iβ." The process as claimed in claim 15 wherein the solid preparation 'is in the dosage form of tablets, powders, granules or capsules.
17. The process as claimed in any of claims 10 - 16 wherein the stabilized pharmaceutical preparation containing a 4-amino-3-substituted-butanic acid derivative is a gabapentin-cσntaining preparation, a pregabalin-containing preparation, a baclofen-cσntaining preparation, or a preparation containing 3-aιιnσmethyl-4-cyclohexyl-butanoic acid, 3-aminomethyl-5-cyclchexyl-pentanoιc acid, 3- aminomethyl-4-phenyl-butanoic acid or 3-aminomethyl-5- phenyl-pentanoic acid.
PCT/US1999/010190 1998-05-15 1999-05-10 Stabilized pharmaceutical preparations of gamma-aminobutyric acid derivatives and process for preparing the same Ceased WO1999059573A1 (en)

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AU40735/99A AU768277B2 (en) 1998-05-15 1999-05-10 Stabilized pharmaceutical preparations of gamma-aminobutyric acid derivatives and process for preparing the same
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SI9930624T SI1077692T1 (en) 1998-05-15 1999-05-10 Amino acid stabilized gabapentin and pregabalin preparations and process for preparing the same
NZ508015A NZ508015A (en) 1998-05-15 1999-05-10 Stabilized pharmaceutical preparations of gamma- aminobutyric acid derivatives and process for preparing the same
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US09/674,815 US7309719B1 (en) 1998-05-15 1999-05-10 Stabilized pharmaceutical preparation of gamma-aminobutyric acid derivatives and process for preparing the same
DE69918977T DE69918977T2 (en) 1998-05-15 1999-05-10 AMINO ACID-STABILIZED GABAPENTIN AND PREGABALINE PREPARATIONS AND METHOD FOR THE PRODUCTION THEREOF
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EP1294364A4 (en) * 2000-06-16 2004-06-16 Teva Pharma Stable gabapentin having ph within a controlled range
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US9144559B2 (en) 2005-11-02 2015-09-29 Warner-Lambert Company Llc Solid pharmaceutical compositions containing pregabalin
US10022447B2 (en) 2005-11-02 2018-07-17 Warner-Lambert Company Llc Solid pharmaceutical compositions containing pregabalin
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US20100196465A1 (en) * 2007-07-11 2010-08-05 Pierre Fabre Medicament Stable pharmaceutical composition of a water-soluble vinorelbine salt
EP2389933A1 (en) 2010-05-25 2011-11-30 Sanovel Ilac Sanayi ve Ticaret A.S. Controlled-Release Pregabalin Compositions
EP2389934A1 (en) 2010-05-25 2011-11-30 Sanovel Ilac Sanayi ve Ticaret A.S. Controlled-Release Tablet Formulations of Pregabalin
EP2389935A1 (en) 2010-05-25 2011-11-30 Sanovel Ilac Sanayi ve Ticaret A.S. Controlled-Release oral Solution Formulations of Pregabalin
EP2929878A1 (en) * 2014-04-09 2015-10-14 Arven Ilac Sanayi ve Ticaret A.S. Extended release formulations of gabapentin
US10561602B2 (en) 2015-05-26 2020-02-18 Isa Odidi Controlled extended release pregabalin

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