WO2000071098A1 - A pharmaceutical composition containing an active agent that is maintained in solid amorphous form and method of making the same - Google Patents

A pharmaceutical composition containing an active agent that is maintained in solid amorphous form and method of making the same Download PDF

Info

Publication number
WO2000071098A1
WO2000071098A1 PCT/US2000/014049 US0014049W WO0071098A1 WO 2000071098 A1 WO2000071098 A1 WO 2000071098A1 US 0014049 W US0014049 W US 0014049W WO 0071098 A1 WO0071098 A1 WO 0071098A1
Authority
WO
WIPO (PCT)
Prior art keywords
solvent
active agent
composition
amorphous form
crospovidone
Prior art date
Application number
PCT/US2000/014049
Other languages
French (fr)
Inventor
Jinling Chen
Zalman Vilkov
Original Assignee
Purepac Pharmaceutical Co.
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Purepac Pharmaceutical Co. filed Critical Purepac Pharmaceutical Co.
Priority to EP00936175A priority Critical patent/EP1185251A1/en
Priority to AU51529/00A priority patent/AU5152900A/en
Publication of WO2000071098A1 publication Critical patent/WO2000071098A1/en

Links

Classifications

    • 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
    • A61K9/141Intimate drug-carrier mixtures characterised by the carrier, e.g. ordered mixtures, adsorbates, solid solutions, eutectica, co-dried, co-solubilised, co-kneaded, co-milled, co-ground products, co-precipitates, co-evaporates, co-extrudates, co-melts; Drug nanoparticles with adsorbed surface modifiers
    • A61K9/146Intimate drug-carrier mixtures characterised by the carrier, e.g. ordered mixtures, adsorbates, solid solutions, eutectica, co-dried, co-solubilised, co-kneaded, co-milled, co-ground products, co-precipitates, co-evaporates, co-extrudates, co-melts; Drug nanoparticles with adsorbed surface modifiers with organic macromolecular compounds
    • 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
    • A61K47/50Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates
    • A61K47/51Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent
    • A61K47/56Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent the modifying agent being an organic macromolecular compound, e.g. an oligomeric, polymeric or dendrimeric molecule

Definitions

  • This invention relates to a pharmaceutical composition containing active agents which are maintained in a solid amorphous form.
  • Drug substances ranging from slightly or sparingly soluble to insoluble, have been found to decrease in crystallinity when mixed with various polymers and diluents.
  • Sekizaki et al., Chem. Pharm. Bull , 43(6):988-993 (1995) it was found that ibuprofen became amorphous when the crystalline powder was mixed with polyvinylpyrrolidone.
  • Kaneniwa et al. Chem. Pharm. Bull , 26(9): 2734-2743 (1978) a decrease in crystallinity was observed when amobarbital was treated in the presence of diluents. This decrease in crystallinity can enhance the solubility, dissolution rates and bioavailability of these substances.
  • the amorphous form of drug substances are generally unstable, and can convert to a crystalline form.
  • Some investigators have attempted to stabilize the amorphous form of drug substances by utilizing solid dispersion techniques. For example, in Imaizumi et al. , Chem. Pharm. Bull. , 31(7): 2510- 2512 (1983), the stability of the amorphous form of indomethacin was enhanced by solid dispersion of the indomethacin in polyvinylpolypyrrolidone. Additionally, in Thakkar et al., J. Pharm.
  • WO 99/00131 published on January 7, 1999, teaches a process for preparing a solid state dispersion of paroxetine or its acid addition salts using a solvent or fusion process.
  • paroxetine free base is dissolved in a polymer/solvent solution, contacted with dry hydrochloride gas and then the non-aqueous solvent is removed by evaporation under vacuum.
  • Preparation of a solid state dispersion, by the fusion technique is taught to involve mixing a polymer with paroxetine free base, melting the mixture, contacting the melt with dry hydrogen chloride and then cooling the mixture.
  • WO 99/00131 does not teach the use of a complexing agent to reduce and/or destroy the crystallinity of the crystalline form of an active drug nor does it teach the use of a co-solvent to prevent and/or reduces recrystallization.
  • pharmaceutically active agents in crystalline form, can be combined with a complexing agent and a co-solvent in order for the active agents to be converted to and maintained in a solid amorphous form.
  • one aspect of the present invention is a pharmaceutical composition
  • a pharmaceutical composition comprising: an active agent in solid amorphous form, a complexing agent, and a non- volatile co-solvent; wherein the complexing agent converts the active agent from crystalline form to solid amorphous form, and the active agent, in the absence of the co- solvent, can recrystallize in the presence of the complexing agent.
  • a first preferred embodiment of the invention is that the active agent is a drug substance, preferably in crystalline form prior to its conversion to amorphous form. More preferably, the active agent is paroxetine, salts of paroxetine, spironolactone, etodolac, diclofenac or salts of diclofenac.
  • a second preferred embodiment of the invention is that the complexing agent is selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof.
  • a third preferred embodiment of the invention is that the non-volatile co- solvent is compatible with the active agent and miscible with the solvent.
  • a more preferred embodiment is that the co-solvent is polyethylene glycol.
  • a fourth preferred embodiment is that the solvent is either an organic and volatile substance or water.
  • the organic and volatile solvent is selected from the group consisting of ethanol, methanol, acetone, methylene chloride and a combination thereof.
  • An additional aspect of the invention is a pharmaceutical composition
  • a pharmaceutical composition comprising: paroxetine hydrochloride in a solid amorphous form, a complexing agent selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof, and polyethylene glycol 300.
  • a further aspect of the invention is a method for producing a pharmaceutical composition which comprises an active agent that is maintained in a solid amorphous form, comprising: mixing a crystalline form of an active agent with a solvent; adding a complexing agent and a co-solvent to the mixture; and removing the solvent from the mixture so as to obtain the active agent in solid amorphous form.
  • Another aspect of the invention is a method for producing a pharmaceutical composition which comprises paroxetine hydrochloride that is maintained in a solid amorphous form, comprising: mixing a crystalline form of paroxetine hydrochloride with ethanol; adding a complexing agent selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof, and polyethylene glycol 300 to the mixture; and removing the ethanol from the mixture so as to obtain the paroxetine hydrochloride in solid amorphous form.
  • Figure 1 represents the results of DSC run of paroxetine hydrochloride anhydrate showing a peak at 115° C, the melting point of the crystal.
  • Figure 2 represents the results of a DSC run on a sample containing a 1:3 ratio of paroxetine hydrochloride .-crospovidone (Sample 1).
  • Figure 3 represents the results of a DSC run on a sample containing a 1:3: 1 ratio of paroxetine hydrochloride: crospovidone: PEG 300 (Sample 2).
  • Figure 4 represents the results of a DSC run on a sample containing a 1: 10 ratio of paroxetine hydrochloride: crospovidone (Sample 3).
  • Figure 5 represents the results of a DSC run on a sample containing a 1: 10: 1 ratio of paroxetine hydrochloride: crospovidone: PEG 300 (Sample 4).
  • Figure 6 represents the results of a DSC run on a sample containing a 1:3 ratio of paroxetine hydrochloride: crospovidone that was mixed with a spatula (Sample 5).
  • Figure 7 represents the results of a DSC run on a sample containing a 1:2: 1: 1 ratio of paroxetine hydrochloride: crospovidone: povidone: PEG 300.
  • Figure 8 represents the results of DSC run of spironolactone showing a melting range of the crystal at 198-207 °C, the melting point of the crystal.
  • Figure 9 represents the results of a DSC run on a sample containing a 1:3 ratio of spironolactone: crospovidone (Sample 6).
  • Figure 10 represents the results of a DSC run on a sample containing a 1:3: 1 ratio of spironolactone : crospovidone : PEG 300 (Sample 7) .
  • Figure 11 represents the results of DSC run of etodolac showing a melting range of the crystal at 146-151 °C.
  • Figure 12 represents the results of a DSC run on a sample containing a 1: 1:3: 1 ratio of etodolac: povidone: crospovidone: PEG 300.
  • Figure 13 represents the results of DSC run of diclofenac sodium showing a melting range of the crystal at 283-285 °C.
  • Figure 14 represents the results of a DSC run on a sample containing a 1 : 1:3: 1 ratio of diclofenac sodium:povidone:crospoviddone:PEG 300.
  • the inventors have surprisingly found that active agents in solid amorphous form, which can recrystallize in the presence of a complexing agent, can be stabilized or maintained in its amorphous state by combining the amorphous form of the active agent with a complexing agent and a co-solvent.
  • active agent is defined as an active ingredient that is intended for use in the diagnosis, cure, mitigation, treatment or prevention of disease in humans or other animals.
  • active agents include, but are not limited to, crystalline forms of active agents which have appreciable solubilities in a solvent wherein the solvent is ultimately removed from the final product.
  • the solvent is preferably either an organic and volatile substance or water. More preferably, the organic and volatile solvent includes, but is not limited to, ethanol, methanol, acetone, methylene chloride or a combination thereof.
  • the active agents of the present invention also include drug substances such as paroxetine, salts of paroxetine (e.g., acid addition salts such as paroxetine hydrochloride), spironolactone, etodolac, diclofenac and salts of diclofenac (e.g., sodium or potassium salts of diclofenac).
  • drug substances such as paroxetine, salts of paroxetine (e.g., acid addition salts such as paroxetine hydrochloride), spironolactone, etodolac, diclofenac and salts of diclofenac (e.g., sodium or potassium salts of diclofenac).
  • Other active agents will be recognized by those skilled in the art.
  • the active agent is present in a pharmacologically effective amount.
  • a pharmacologically effective amount is any amount of active agent sufficient to provide pharmacological activity or otherwise sufficient to affect the structure or function of the body in humans or other animals.
  • paroxetine and its salts e.g., acid addition salts
  • paroxetine and its salts are known to have an anti-depressant effect, utility as an analgesic, and an anti-obesity effect.
  • the indications include depression, obsessive compulsive disorders and panic disorders.
  • Spironolactone for example, acts both as a diuretic and as an antihypertensive drug.
  • the indications include primary hyperaldosteronism, edematous conditions, essential hypertension and hypokalemia.
  • the drug substance etodolac is, for instance, a nonsteroidal anti- inflammatory drug that exhibits anti-inflammatory, analgesic and antipyretic activies.
  • the indications include acute and long term use for osteoarthritis and rheumatoid arthritis and management of pain.
  • Diclofenac and its salts are also nonsteroidal anti-inflammatory drugs that exhibit the same properties as listed for etodolac.
  • Diclofenac and its salts are used to treat osteoarthritis, rheumatoid arthritis, ankylosing spondylitis, management of pain and primary dysmenorrhea. Other pharmacological activities will be recognied by one skilled in the art.
  • an effective amount depends on various factors well known to those skilled in the art such as the nature and severity of the condition to be treated, the frequency and route of administration, and the weight of the human or animal requiring treatment. However, it is believed that an amount from about 0.01 to 100 mg/kg of body weight per day of any one of the preferred active agents should be effective for producing the intended pharmacological effect.
  • the pharmaceutical composition of the present invention can be presented as a unit dose.
  • a unit dose of the pharmaceutical composition containing any one of the preferred active agents can generally contain from about 0.1 to 1000 mg of the active agent.
  • Such unit dose compositions may be administered once or more times a day. It is to be understood that the amounts set forth herein are exemplary and they do not, to any extent, limit the scope or practice of the invention.
  • complexing agent is a substance which associates with the active agent through either chemical binding or physical interaction to reduce or destroy the crystallinity of the active agent.
  • the complexing agent is crospovidone, povidone, cyclodextrin or any combination thereof.
  • a preferred amount of complexing agent to be used in the present invention ranges from 10/1 - 1/100 wt/wt (drug/complexing agent). Parameters which may affect the ratio include molecular weights of the drug and the complexing agent as well as the molecular structure of the drug and the complexing agent.
  • a co-solvent is defined as a substance which has an appreciable solubility for the drug substance and which enhances the complexation and/or stabilizes the complex formed.
  • the co-solvent should be nonvolatile. Non- volatile means that there should not be a significant amount of co- solvent loss under processing conditions, including the process to remove the solvent.
  • the co-solvent should be compatible with the active agent and miscible with the solvent.
  • co-solvents include, but are not limited to, polyethylene glycols, propylene glycol, glycerol, liquid petrolatum and lauryl alcohol. Other co-solvents will be apparent to those skilled in the art.
  • a preferred amount of co-solvent to be used in the present invention ranges from 10/1 - 1/10 wt/wt (drug/co-solvent).
  • the range of co-solvent may depend on the type of drug, complexing agent and co-solvent used.
  • compositions according the present invention can also include other inert material or additives known as a pharmaceutically acceptable excipient.
  • Pharmaceutically acceptable excipients are generally present to facilitate manufacturing, packaging and handling of the drug. These well known and art recognized excipients include, for example, fillers or diluents, binders or granulators, lubricants, glidants, disintegrants and coloring, flavoring and sweetening agents. Other excipients will be apparent to those of skill in the art.
  • compositions of the present invention are preferably in solid dosage form. Any well known tabletting procedure, encapsulating procedure or other procedure to prepare a solid dosage form can be employed herein.
  • paroxetine hydrochloride The following procedure was used to prepare a solid amorphous form of paroxetine hydrochloride. To begin, 10 grams of anhydrous paroxetine hydrochloride were added to 120 grams of ethanol. The sample was stirred and heated to 45 °C. Stirring was continued until the paroxetine hydrochloride was fully dissolved. Crospovidone, 30 grams of Polyplasdone XL (BASF; Mount Olive, NJ), was added to the paroxetine hydrochloride solution to form a slurry. The slurry was stirred and heated at 45 °C for 24 hours. Polyethylene glycol, 10 grams of PEG 300 (Dow Chemicals; Midland, Michigan), was added to the slurry and the sample was mixed well.
  • Crospovidone 30 grams of Polyplasdone XL (BASF; Mount Olive, NJ)
  • a solid paroxetine hydrochloride containing drug complex, wherein the paroxetine hydrochloride is maintained in an amorphous form is as follows:
  • a solid spironolatone containing drug complex, wherein the spironolactone is maintained in an amorphous form is as follows:
  • the above drug complexes can be prepared using the following steps.
  • the ethanol (solvent) and the active agent are placed in a bowl of a high-shear mixer (Collette Gral), equipped with a heating jacket and connected to the source of heat.
  • the set-point temperature of the heating medium is set to 50 °C.
  • the content of the bowl is heated, while the material is stirred, until all of the active agent is completely dissolved.
  • the povidone is added to the bowl and stirred until it is completely dissolved.
  • the crospovidone is then added and the bowl's content is stirred for two hours.
  • the polyethylene glycol is added next and the stirring continues for 30 minutes.
  • the set-point temperature of the heating medium is set to 80°C (in the event that the solvent is water the set-point temperature of the heating medium would be set for 100°C) and the removal of the solvent is commenced under slight negative pressure, until the consistency of the material is such as to be suitable for transfer to the drying equipment (the solvent content is approximately 15% to 25%).
  • the material is then placed in the drying equipment (a tray oven or a fluid-bed drier) and dried at the inlet air temperature set at 50 °C, until the residual solvent content is less than 5 % .
  • the semi-dried material is milled using a comminuting mill (Fitzpatrick) equipped with a perforated plate with 0.093" diameter holes and set at 2,450 rpm (medium speed).
  • the milled material is then returned back to the drying equipment and dried at 50 °C until the residual moisture content is below 2% .
  • the dried material is milled again through a perforated plate with 0.020" diameter holes with the mill being set at 4,600 rpm (high speed).
  • the complex can be spray dried or vacuum microwave dried. Other methods will be readily recognized by those skilled in the art.
  • the milled granules are placed in a jacketed bowl of a Gral, PEG 8000 (Carbowax) is added and the content of the bowl is heated at 80°C, while mixing, until all of the particles are coated with PEG.
  • PEG 8000 Carbowax
  • the material is then discharged from the bowl, spread on ss trays and allowed to cool to room temperature.
  • the cooled material is milled again through a perforated plate with 0.020" diameter holes with the mill being set at at 4,600 rpm (high speed).
  • a final blend can be prepared which can either be compressed into tablets or filled into empty gelatin capsules.
  • Final blends containing the paroxetine hydrochloride-containing drug complex as well as the spironolactone-containing drug complex are as follows:
  • the above tabletting ingredients are combined in a blender and mixed together to form a final blend.
  • the blend is compressed into tablets which can be optionally color coated with an aqueous dispersion such as Opadry ® (Colorcon).
  • the final blend can be filled into empty gelatin capsules.
  • DSC differential scanning calorimetry
  • Sample 5 is simply a 1:3 ratio of anhydrous paroxetine hydrochloride: crospovidone that was mixed with a spatula.
  • Figures 2- 6 and 9-10 The results of the DSC runs, as described above, are set forth in Figures 2- 6 and 9-10.
  • Figures 1 and 8 demonstrate what the scans of DSC runs look like for the crystalline form of paroxetine hydrochloride and spironolactone.
  • Figures 2, 4 and 6 where the co-solvent is absent, small peaks are present which indicate re-crystallization.
  • Figures 3 and 5 no peaks are shown on the scan.
  • the absence of peaks at the melting temperature of the drug crystals indicates the absence of drug crystals in the sample.
  • the samples containing both the co-solvent and the complexing agent are maintained in a solid amorphous form.
  • EXAMPLE X A solid etodolac-containing drug complex (a 1: 1:3: 1 ratio of etodolac:povidone:crospovidone:PEG 300), was prepared in the following manner.
  • 800 g of micronized etodolac and 8,000 g of ethanol were places in a 25 L Collette Gral bowl and mixed while warming to 50 °C, until all of the drug was dissolved.
  • 800 g of Povidone USP K 29-32 was added and mixed until completely dissolved.
  • 1,600 g of Crospovidone NF was added and mixed for 2 hours while maintaining the termperature at 50°C.
  • 800 g of PEG 300 was added and mixed for 30 minutes. The heating temperature was increased to 80 °C and the bulk of alcohol was evaporated. Semi-dry material was placed in a tray oven and dried at 40°C for approximately 18 hours.
  • the material was then milled through a perforated plate with 0.065" diameter holes using a Fitzpatrick comminuting mill. This material was then placed back in the oven for an additional drying, until the residual solvent content is below 2 % . This material is then milled through a perforated plate with 0.020" diameter holes.
  • a solid diclofenac sodium-containing drug complex (a 1: 1:3: 1 ratio of diclofenac sodium:povidone:crospovidone:PEG 300), was prepared in the following manner .
  • the material was then milled through a perforated plate with 0.065" diameter holes using a Fitzpatrick comminuting mill. This material was then placed back in the oven for an additional drying, until the residual solvent content is below 2% . This material is then milled through a perforated plate with 0.020" diameter holes.

Abstract

A pharmaceutical composition and process for producing a pharmaceutical composition that contains an active agent in solid amorphous form wherein the amorphous form of the active agent is maintained.

Description

A PHARMACEUTICAL COMPOSITION CONTAINING AN ACTIVE
AGENT THAT IS MAINTAINED IN SOLID AMORPHOUS FORM
AND METHOD OF MAKING THE SAME
BACKGROUND OF THE INVENTION 1. Field of the Invention
This invention relates to a pharmaceutical composition containing active agents which are maintained in a solid amorphous form.
2. Description of the Related Art
Drug substances, ranging from slightly or sparingly soluble to insoluble, have been found to decrease in crystallinity when mixed with various polymers and diluents. For example, in Sekizaki et al., Chem. Pharm. Bull , 43(6):988-993 (1995), it was found that ibuprofen became amorphous when the crystalline powder was mixed with polyvinylpyrrolidone. In Kaneniwa et al. Chem. Pharm. Bull , 26(9): 2734-2743 (1978), a decrease in crystallinity was observed when amobarbital was treated in the presence of diluents. This decrease in crystallinity can enhance the solubility, dissolution rates and bioavailability of these substances.
The amorphous form of drug substances, however, are generally unstable, and can convert to a crystalline form. Some investigators have attempted to stabilize the amorphous form of drug substances by utilizing solid dispersion techniques. For example, in Imaizumi et al. , Chem. Pharm. Bull. , 31(7): 2510- 2512 (1983), the stability of the amorphous form of indomethacin was enhanced by solid dispersion of the indomethacin in polyvinylpolypyrrolidone. Additionally, in Thakkar et al., J. Pharm. Pharmac , 29:783-784 (1977), it was reported that the conversion to a crystalline state was effectively prevented when nabilone was dispersed in the water-soluble matrix of polyvinylpyrrolidone. United States Patent No. 5,672,612, issued to Ronsen et al. on September 30, 1997, discloses the preparation of an amorphous form of paroxetine hydrochloride. Unlike the present invention, the Ronsen et al. patent, discloses combining paroxetine free base with a hydrochloric acid/ethanol solution and drying the product. Thus, the Rosen et al. patent does not address the problem solved by the present invention, that is converting a crystalline form of an active agent into a stable amorphous form.
WO 99/00131, published on January 7, 1999, teaches a process for preparing a solid state dispersion of paroxetine or its acid addition salts using a solvent or fusion process. In the solvent method, paroxetine free base is dissolved in a polymer/solvent solution, contacted with dry hydrochloride gas and then the non-aqueous solvent is removed by evaporation under vacuum. Preparation of a solid state dispersion, by the fusion technique, is taught to involve mixing a polymer with paroxetine free base, melting the mixture, contacting the melt with dry hydrogen chloride and then cooling the mixture. WO 99/00131 does not teach the use of a complexing agent to reduce and/or destroy the crystallinity of the crystalline form of an active drug nor does it teach the use of a co-solvent to prevent and/or reduces recrystallization.
Despite certain attempts, there still exists a need in the art for a pharmaceutical composition containing an active agent in a solid amorphous form wherein the active agent is maintained in such a form.
BRIEF SUMMARY OF THE INVENTION
It has been discovered that pharmaceutically active agents, in crystalline form, can be combined with a complexing agent and a co-solvent in order for the active agents to be converted to and maintained in a solid amorphous form.
Thus, one aspect of the present invention is a pharmaceutical composition comprising: an active agent in solid amorphous form, a complexing agent, and a non- volatile co-solvent; wherein the complexing agent converts the active agent from crystalline form to solid amorphous form, and the active agent, in the absence of the co- solvent, can recrystallize in the presence of the complexing agent.
A first preferred embodiment of the invention is that the active agent is a drug substance, preferably in crystalline form prior to its conversion to amorphous form. More preferably, the active agent is paroxetine, salts of paroxetine, spironolactone, etodolac, diclofenac or salts of diclofenac.
A second preferred embodiment of the invention is that the complexing agent is selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof.
A third preferred embodiment of the invention is that the non-volatile co- solvent is compatible with the active agent and miscible with the solvent. A more preferred embodiment is that the co-solvent is polyethylene glycol.
A fourth preferred embodiment is that the solvent is either an organic and volatile substance or water. An even more preferred embodiment is that the organic and volatile solvent is selected from the group consisting of ethanol, methanol, acetone, methylene chloride and a combination thereof.
An additional aspect of the invention is a pharmaceutical composition comprising: paroxetine hydrochloride in a solid amorphous form, a complexing agent selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof, and polyethylene glycol 300. A further aspect of the invention is a method for producing a pharmaceutical composition which comprises an active agent that is maintained in a solid amorphous form, comprising: mixing a crystalline form of an active agent with a solvent; adding a complexing agent and a co-solvent to the mixture; and removing the solvent from the mixture so as to obtain the active agent in solid amorphous form.
Another aspect of the invention is a method for producing a pharmaceutical composition which comprises paroxetine hydrochloride that is maintained in a solid amorphous form, comprising: mixing a crystalline form of paroxetine hydrochloride with ethanol; adding a complexing agent selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof, and polyethylene glycol 300 to the mixture; and removing the ethanol from the mixture so as to obtain the paroxetine hydrochloride in solid amorphous form.
With the foregoing and other objects, advantages and features of the invention that will become hereinafter apparent, the nature of the invention may be more clearly understood by reference to the following detailed description and to the appended claims.
BRIEF DESCRIPTION OF THE DRAWINGS
Figure 1 represents the results of DSC run of paroxetine hydrochloride anhydrate showing a peak at 115° C, the melting point of the crystal.
Figure 2 represents the results of a DSC run on a sample containing a 1:3 ratio of paroxetine hydrochloride .-crospovidone (Sample 1).
Figure 3 represents the results of a DSC run on a sample containing a 1:3: 1 ratio of paroxetine hydrochloride: crospovidone: PEG 300 (Sample 2). Figure 4 represents the results of a DSC run on a sample containing a 1: 10 ratio of paroxetine hydrochloride: crospovidone (Sample 3).
Figure 5 represents the results of a DSC run on a sample containing a 1: 10: 1 ratio of paroxetine hydrochloride: crospovidone: PEG 300 (Sample 4). Figure 6 represents the results of a DSC run on a sample containing a 1:3 ratio of paroxetine hydrochloride: crospovidone that was mixed with a spatula (Sample 5).
Figure 7 represents the results of a DSC run on a sample containing a 1:2: 1: 1 ratio of paroxetine hydrochloride: crospovidone: povidone: PEG 300. Figure 8 represents the results of DSC run of spironolactone showing a melting range of the crystal at 198-207 °C, the melting point of the crystal.
Figure 9 represents the results of a DSC run on a sample containing a 1:3 ratio of spironolactone: crospovidone (Sample 6).
Figure 10 represents the results of a DSC run on a sample containing a 1:3: 1 ratio of spironolactone : crospovidone : PEG 300 (Sample 7) .
Figure 11 represents the results of DSC run of etodolac showing a melting range of the crystal at 146-151 °C.
Figure 12 represents the results of a DSC run on a sample containing a 1: 1:3: 1 ratio of etodolac: povidone: crospovidone: PEG 300. Figure 13 represents the results of DSC run of diclofenac sodium showing a melting range of the crystal at 283-285 °C.
Figure 14 represents the results of a DSC run on a sample containing a 1 : 1:3: 1 ratio of diclofenac sodium:povidone:crospoviddone:PEG 300.
DETAILED DESCRIPTION OF THE INVENTION The decrease in crystallinity of various drug substances can enhance the solubility, dissolution rates and bioavailability of these substances. Therefore, use of the amorphous form of these drug substances in pharmaceutical formulations is often advantageous. The amorphous form of these drug substances, however, is unstable, and can convert to a crystalline form.
Despite the prior art which teaches that when the amorphous forms of indomethacin and nabilone were dispersed in either polyvinylpyrrolidone (also known as PVP or povidone) or polyvinylpolypyrrolidone (also known as PNPP or crospovidone) the amorphous state of the drug substances were stabilized, the inventors of the subject application have determined that a number of active agents in their amorphous form can recrystallize in the presence of a complexing agent. The inventors have surprisingly found that active agents in solid amorphous form, which can recrystallize in the presence of a complexing agent, can be stabilized or maintained in its amorphous state by combining the amorphous form of the active agent with a complexing agent and a co-solvent.
This invention is applicable to any solid active agent. The term active agent is defined as an active ingredient that is intended for use in the diagnosis, cure, mitigation, treatment or prevention of disease in humans or other animals. Such active agents include, but are not limited to, crystalline forms of active agents which have appreciable solubilities in a solvent wherein the solvent is ultimately removed from the final product. The solvent is preferably either an organic and volatile substance or water. More preferably, the organic and volatile solvent includes, but is not limited to, ethanol, methanol, acetone, methylene chloride or a combination thereof. The active agents of the present invention also include drug substances such as paroxetine, salts of paroxetine (e.g., acid addition salts such as paroxetine hydrochloride), spironolactone, etodolac, diclofenac and salts of diclofenac (e.g., sodium or potassium salts of diclofenac). Other active agents will be recognized by those skilled in the art.
The active agent is present in a pharmacologically effective amount. A pharmacologically effective amount, as used herein, is any amount of active agent sufficient to provide pharmacological activity or otherwise sufficient to affect the structure or function of the body in humans or other animals.
The specific pharmacological activity will depend upon the particular active agent which is utilized. For instance, paroxetine and its salts, e.g., acid addition salts, are known to have an anti-depressant effect, utility as an analgesic, and an anti-obesity effect. The indications include depression, obsessive compulsive disorders and panic disorders. Spironolactone, for example, acts both as a diuretic and as an antihypertensive drug. The indications include primary hyperaldosteronism, edematous conditions, essential hypertension and hypokalemia. The drug substance etodolac is, for instance, a nonsteroidal anti- inflammatory drug that exhibits anti-inflammatory, analgesic and antipyretic activies. The indications include acute and long term use for osteoarthritis and rheumatoid arthritis and management of pain. Diclofenac and its salts are also nonsteroidal anti-inflammatory drugs that exhibit the same properties as listed for etodolac. Diclofenac and its salts are used to treat osteoarthritis, rheumatoid arthritis, ankylosing spondylitis, management of pain and primary dysmenorrhea. Other pharmacological activities will be recognied by one skilled in the art.
Determination of an effective amount depends on various factors well known to those skilled in the art such as the nature and severity of the condition to be treated, the frequency and route of administration, and the weight of the human or animal requiring treatment. However, it is believed that an amount from about 0.01 to 100 mg/kg of body weight per day of any one of the preferred active agents should be effective for producing the intended pharmacological effect.
The pharmaceutical composition of the present invention can be presented as a unit dose. Thus, a unit dose of the pharmaceutical composition containing any one of the preferred active agents can generally contain from about 0.1 to 1000 mg of the active agent. Such unit dose compositions may be administered once or more times a day. It is to be understood that the amounts set forth herein are exemplary and they do not, to any extent, limit the scope or practice of the invention.
The term "complexing agent" as defined in the present invention is a substance which associates with the active agent through either chemical binding or physical interaction to reduce or destroy the crystallinity of the active agent. Preferrably, the complexing agent is crospovidone, povidone, cyclodextrin or any combination thereof. This invention is not limited, however, to a particular complexing agent and other complexing agents will be apparent to those skilled in the art. A preferred amount of complexing agent to be used in the present invention ranges from 10/1 - 1/100 wt/wt (drug/complexing agent). Parameters which may affect the ratio include molecular weights of the drug and the complexing agent as well as the molecular structure of the drug and the complexing agent. Further, as used herein, a co-solvent is defined as a substance which has an appreciable solubility for the drug substance and which enhances the complexation and/or stabilizes the complex formed. Generally, the co-solvent should be nonvolatile. Non- volatile means that there should not be a significant amount of co- solvent loss under processing conditions, including the process to remove the solvent. Preferably, the co-solvent should be compatible with the active agent and miscible with the solvent. Such co-solvents include, but are not limited to, polyethylene glycols, propylene glycol, glycerol, liquid petrolatum and lauryl alcohol. Other co-solvents will be apparent to those skilled in the art.
A preferred amount of co-solvent to be used in the present invention ranges from 10/1 - 1/10 wt/wt (drug/co-solvent). The range of co-solvent may depend on the type of drug, complexing agent and co-solvent used.
The pharmaceutical compositions according the present invention can also include other inert material or additives known as a pharmaceutically acceptable excipient. Pharmaceutically acceptable excipients are generally present to facilitate manufacturing, packaging and handling of the drug. These well known and art recognized excipients include, for example, fillers or diluents, binders or granulators, lubricants, glidants, disintegrants and coloring, flavoring and sweetening agents. Other excipients will be apparent to those of skill in the art.
The pharmaceutical compositions of the present invention are preferably in solid dosage form. Any well known tabletting procedure, encapsulating procedure or other procedure to prepare a solid dosage form can be employed herein.
The following examples are presented in order to more fully illustrate the preferred embodiments of the invention. They should in no way be construed, however, as limiting the scope of the invention.
EXAMPLE I
The following procedure was used to prepare a solid amorphous form of paroxetine hydrochloride. To begin, 10 grams of anhydrous paroxetine hydrochloride were added to 120 grams of ethanol. The sample was stirred and heated to 45 °C. Stirring was continued until the paroxetine hydrochloride was fully dissolved. Crospovidone, 30 grams of Polyplasdone XL (BASF; Mount Olive, NJ), was added to the paroxetine hydrochloride solution to form a slurry. The slurry was stirred and heated at 45 °C for 24 hours. Polyethylene glycol, 10 grams of PEG 300 (Dow Chemicals; Midland, Michigan), was added to the slurry and the sample was mixed well. The sample was then dried in an oven at 55 °C to remove the ethanol. The weight of the sample was monitored periodically until a constant weight was achieved. The sample was removed from the oven and ground to obtain a solid material containing of the amorphous form of paroxetine hydrochloride. EXAMPLE II
A solid paroxetine hydrochloride containing drug complex, wherein the paroxetine hydrochloride is maintained in an amorphous form, is as follows:
Figure imgf000011_0001
A solid spironolatone containing drug complex, wherein the spironolactone is maintained in an amorphous form, is as follows:
Figure imgf000011_0002
The above drug complexes can be prepared using the following steps. The ethanol (solvent) and the active agent are placed in a bowl of a high-shear mixer (Collette Gral), equipped with a heating jacket and connected to the source of heat. The set-point temperature of the heating medium is set to 50 °C. The content of the bowl is heated, while the material is stirred, until all of the active agent is completely dissolved. The povidone is added to the bowl and stirred until it is completely dissolved. The crospovidone is then added and the bowl's content is stirred for two hours. The polyethylene glycol is added next and the stirring continues for 30 minutes. The set-point temperature of the heating medium is set to 80°C (in the event that the solvent is water the set-point temperature of the heating medium would be set for 100°C) and the removal of the solvent is commenced under slight negative pressure, until the consistency of the material is such as to be suitable for transfer to the drying equipment (the solvent content is approximately 15% to 25%). The material is then placed in the drying equipment (a tray oven or a fluid-bed drier) and dried at the inlet air temperature set at 50 °C, until the residual solvent content is less than 5 % . The semi-dried material is milled using a comminuting mill (Fitzpatrick) equipped with a perforated plate with 0.093" diameter holes and set at 2,450 rpm (medium speed). The milled material is then returned back to the drying equipment and dried at 50 °C until the residual moisture content is below 2% . The dried material is milled again through a perforated plate with 0.020" diameter holes with the mill being set at 4,600 rpm (high speed).
Alternative techniques can also be used to dry the complex. In addition to oven and fluid bed drying, the complex can be spray dried or vacuum microwave dried. Other methods will be readily recognized by those skilled in the art.
These next steps are optional. The milled granules are placed in a jacketed bowl of a Gral, PEG 8000 (Carbowax) is added and the content of the bowl is heated at 80°C, while mixing, until all of the particles are coated with PEG. The material is then discharged from the bowl, spread on ss trays and allowed to cool to room temperature. The cooled material is milled again through a perforated plate with 0.020" diameter holes with the mill being set at at 4,600 rpm (high speed).
Once the drug complex is formed, a final blend can be prepared which can either be compressed into tablets or filled into empty gelatin capsules. Final blends containing the paroxetine hydrochloride-containing drug complex as well as the spironolactone-containing drug complex are as follows:
Figure imgf000013_0001
The above tabletting ingredients are combined in a blender and mixed together to form a final blend. The blend is compressed into tablets which can be optionally color coated with an aqueous dispersion such as Opadry® (Colorcon). Alternatively, the final blend can be filled into empty gelatin capsules.
EXAMPLES III - IX
To demonstrate that the co-solvent prevents recrystallization of the active agent in the presence of the complexing agent, samples were prepared with and without PEG 300 and then differential scanning calorimetry (DSC) was carried out. The DSC conditions were as follows:
• DSC instrument: Mettler Toledo DSC 821e
• Heating rate: 20° C/minute
• Temperature range: 0° C - 250° C.
The DSC method as described in Imaizumi et al. , Chem. Pharm. Bull. , 28:2565- 2569 (1980) can also be employed for determining the degree of crystallinity of a compound. This article is hereby incorporated by reference in its entirety.
The samples used to run the DSC scans were prepared as follows. Sample 1 - paroxetine hydrochloride: crospovidone = 1:3 Sample 2 - paroxetine hydrochloride: crospovidone: PEG 300 = 1:3: 1 Preparation:
1. 0.5 grams of anhydrous paroxetine hydrochloride was mixed and dissolved in 15 grams of ethanol.
2. 1.5 grams of crospovidone was added to the solution to form a slurry. The slurry was stirred for 2 hours and then sat overnight at room temperature. The slurry was then divided into two equal parts, Sample 1 and Sample 2. 3. Sample 1 was dried in an oven at 45 °C until the ethanol evaporated. The sample was ground and scanned on a DSC.
4. Prior to drying Sample 2, 0.25 grams of PEG 300 was added and mixed. The mixture was then dried at 45 °C until the ethanol evaporated. The sample was ground and scanned on a DSC.
Sample 3 - paroxetine hydrochloride: crospovidone = 1: 10 Sample 4 - paroxetine hydrochlorie: crospovidone: PEG 300 = 1 : 10: 1 Preparation:
The above process was used to produce Samples 3 and 4 with the exception of the change in weight ratios.
Sample 5 - paroxetine hydrochloride: crospovidone = 1 :3 Preparation:
Sample 5 is simply a 1:3 ratio of anhydrous paroxetine hydrochloride: crospovidone that was mixed with a spatula.
Sample 6 - spironolactone: crospovidone = 1:3
Sample 7 - spironolactone: crospovidone: PEG 300 = 1:3: 1 Preparation:
1. 23 grams of spironolactone is added to 230 grams of ethanol. The solution is heated to 50 °C and stirred until the drug is dissolved. 2. 69 grams of crospovidone and an additional 100 grams of ethanol are added to the solution to form a slurry. The mixture is stirred for 24 hours at 50 °C. The slurry is divided into two equal parts, Sample 1 and Sample 2. 3. Sample 1 is dryed at 60 °C until the ethanol has evaporated. The sample is ground and scanned on a DSC. 4. Prior to drying Sample 2, 23 grams of PEG 300 is added and mixed. The mixture is then dryed at 60 °C until the ethanol has evaporated. The sample is ground and scanned on a DSC.
The results of the DSC runs, as described above, are set forth in Figures 2- 6 and 9-10. Figures 1 and 8 demonstrate what the scans of DSC runs look like for the crystalline form of paroxetine hydrochloride and spironolactone. As can be seen from the DSC scans of Figures 2, 4 and 6, where the co-solvent is absent, small peaks are present which indicate re-crystallization. In contrast, the samples where the co-solvent and complexing agent was used, Figures 3 and 5, no peaks are shown on the scan. The absence of peaks at the melting temperature of the drug crystals indicates the absence of drug crystals in the sample. Thus, the samples containing both the co-solvent and the complexing agent are maintained in a solid amorphous form.
EXAMPLE X A solid etodolac-containing drug complex (a 1: 1:3: 1 ratio of etodolac:povidone:crospovidone:PEG 300), was prepared in the following manner.
800 g of micronized etodolac and 8,000 g of ethanol were places in a 25 L Collette Gral bowl and mixed while warming to 50 °C, until all of the drug was dissolved. 800 g of Povidone USP K 29-32 was added and mixed until completely dissolved. 1,600 g of Crospovidone NF was added and mixed for 2 hours while maintaining the termperature at 50°C. 800 g of PEG 300 was added and mixed for 30 minutes. The heating temperature was increased to 80 °C and the bulk of alcohol was evaporated. Semi-dry material was placed in a tray oven and dried at 40°C for approximately 18 hours. The material was then milled through a perforated plate with 0.065" diameter holes using a Fitzpatrick comminuting mill. This material was then placed back in the oven for an additional drying, until the residual solvent content is below 2 % . This material is then milled through a perforated plate with 0.020" diameter holes.
A sample of the resultant complex was tested by DSC and the results are set forth in Figure 12. The Figure shows no peaks, as compared to the crystalline form of the active drug (Figure 11), thereby indicating that the active drug is maintained in solid amorphous form.
EXAMPLE XI
A solid diclofenac sodium-containing drug complex (a 1: 1:3: 1 ratio of diclofenac sodium:povidone:crospovidone:PEG 300), was prepared in the following manner .
1000 g of diclofenac sodium and 10,000 g of purified water were places in a 25 L Collette Gral bowl and mixed while warming to 65 °C, until all of the drug was dissolved. 1,000 g of Povidone USP K 29-32 was added and mixed until completely dissolved. 2,000 g of Crospovidone NF was added and mixed for 2 hours while maintaining the termperature at 65 °C. 1,000 g of PEG 300 was added and mixed for 30 minutes. The heating temperature was increased to 105 °C and the bulk of water was evaporated. Semi-dry material was placed in a tray oven and dried at 55 °C for approximately 18 hours. The material was then milled through a perforated plate with 0.065" diameter holes using a Fitzpatrick comminuting mill. This material was then placed back in the oven for an additional drying, until the residual solvent content is below 2% . This material is then milled through a perforated plate with 0.020" diameter holes.
A sample of the resultant complex was tested by DSC and the results are set forth in Figure 14. The Figure shows no peaks, as compared to the crystalline form of the active drug (Figure 13), thereby indicating that the active drug is maintained in solid amorphous form. While the invention has been described in terms of various preferred embodiments, a person skilled in the art will appreciate that various modifications, substitutions, omissions and changes can be made without departing from the spirit thereof. Accordingly, it is intended that the scope of the present invention be limited solely by the scope of the following claims, including equivalents thereof. Further, all of the publications and patents cited herein are incorporated by reference in their entirety.

Claims

WHAT IS CLAIMED IS:
1. A pharmaceutical composition comprising: an active agent in solid amorphous form, a complexing agent, and a non-volatile co-solvent; wherein the complexing agent converts the active agent from crystalline form to solid amorphous form, and the active agent, in the absence of the co- solvent, can recrystallize in the presence of the complexing agent.
2. The composition of claim 1, wherein the active agent is paroxetine.
3. The composition of claim 1, wherein the active agent is paroxetine hydrochloride.
4. The composition of claim 1, wherein the active agent is spironolactone.
5. The composition of claim 1, wherein the active agent is etodolac.
6. The composition of claim 1, wherein the active agent is diclofenac.
7. The composition of claim 1, wherein the active agent is a sodium or potassium salt of diclofenac.
8. The composition of claim 1, wherein the complexing agent is selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof.
9. The composition of claim 1, wherein the complexing agent is crospovidone.
10. The composition of claim 1, wherein the crystalline form of the active agent is mixed with a solvent which is ultimately removed from the composition.
11. The composition of claim 1 , wherein the solvent is an organic and volatile substance or water.
12. The composition of claim 1, wherein the solvent is selected from the group consisting of ethanol, methanol, acetone, methylene chloride and a combination thereof.
13. The composition of claim 1, wherein the solvent is ethanol.
14. The composition of claim 1, wherein the non-volatile co-solvent is compatible with the active agent and miscible with the solvent.
15. The composition of claim 1, wherein the non- volatile co-solvent is polyethylene glycol .
16. The composition of claim 1, wherein the non-volatile co-solvent is polyethylene glycol 300.
17. The composition of claim 1, wherein the pharmaceutical composition is in a solid dosage form.
18. A pharmaceutical composition comprising: paroxetine hydrochloride in a solid amorphous form, a complexing agent selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof, and polyethylene glycol 300; wherein the complexing agent converts paroxetine hydrochloride from crystalline form to solid amorphous form.
19. The composition of claim 18, wherein the paroxetine hydrochloride is maintained in a solid amorphous form.
20. A method for producing a pharmaceutical composition which comprises an active agent that is maintained in a solid amorphous form, comprising: mixing a crystalline form of an active agent with a solvent; adding a complexing agent and a co-solvent to the mixture; and removing the solvent from the mixture so as to obtain the active agent in solid amorphous form.
21. The method of claim 20, wherein the active agent is paroxetine.
22. The method of claim 20, wherein the active agent is paroxetine hydrochloride.
23. The method of claim 20, wherein the active agent is spironolactone.
24. The method of claim 20, wherein the active agent is etodolac.
25. The method of claim 20, wherein the active agent is diclofenac.
26. The method of claim 20, wherein the active agent is a sodium or potassium salt of diclofenac.
27. The method of claim 20, wherein the solvent is an organic and volatile substance or water.
28. The method of claim 20, wherein the solvent is selected from the group consisting of ethanol, methanol, acetone, methylene chloride and a combination thereof.
29. The method of claim 20, wherein the solvent is ethanol.
30. The method of claim 20, wherein the complexing agent is selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof.
31. The method of claim 20, wherein the complexing agent is crospovidone.
32. The method of claim 20, wherein the non- volatile co-solvent is compatible with the active agent and miscible with the solvent.
33. The method of claim 20, wherein the non- volatile co-solvent is polyethylene glycol.
34. The method of claim 20, wherein the non- volatile co-solvent is polyethylene glycol 300.
35. The pharmaceutical composition produced by the method of claim 20.
36. A method for producing a pharmaceutical composition which comprises paroxetine hydrochloride that is maintained in a solid amorphous form, comprising: mixing a crystalline form of paroxetine hydrochloride with ethanol; adding a complexing agent selected from the group consisting of crospovidone, povidone, cyclodextrin and a combination thereof, and polyethylene glycol 300 to the mixture; and removing the ethanol from the mixture so as to obtain the paroxetine hydrochloride in solid amorphous form.
37. The pharmaceutical composition produced by the method of claim 36.
PCT/US2000/014049 1999-05-24 2000-05-23 A pharmaceutical composition containing an active agent that is maintained in solid amorphous form and method of making the same WO2000071098A1 (en)

Priority Applications (2)

Application Number Priority Date Filing Date Title
EP00936175A EP1185251A1 (en) 1999-05-24 2000-05-23 A pharmaceutical composition containing an active agent that is maintained in solid amorphous form and method of making the same
AU51529/00A AU5152900A (en) 1999-05-24 2000-05-23 A pharmaceutical composition containing an active agent that is maintained in solid amorphous form and method of making the same

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US31744899A 1999-05-24 1999-05-24
US09/317,448 1999-05-24

Publications (1)

Publication Number Publication Date
WO2000071098A1 true WO2000071098A1 (en) 2000-11-30

Family

ID=23233696

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/US2000/014049 WO2000071098A1 (en) 1999-05-24 2000-05-23 A pharmaceutical composition containing an active agent that is maintained in solid amorphous form and method of making the same

Country Status (3)

Country Link
EP (1) EP1185251A1 (en)
AU (1) AU5152900A (en)
WO (1) WO2000071098A1 (en)

Cited By (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP1465601A2 (en) * 2001-12-28 2004-10-13 Teva Pharmaceutical Industries Ltd. A stable pharmaceutical formulation of paroxetine hydrochloride anhydrous and a process for preparation thereof
WO2006119779A2 (en) * 2005-05-10 2006-11-16 Lifecycle Pharma A/S A pharmaceutical composition comprising an aldosterone antagonist in form of solid solution
WO2011130500A1 (en) * 2010-04-16 2011-10-20 Novartis Ag Formulations of a pyridazine bipyrazinyl
WO2011133675A1 (en) * 2010-04-21 2011-10-27 Teva Pharmaceutical Industries Ltd. Gabapentin enacarbil compositions
US8580954B2 (en) 2006-03-28 2013-11-12 Hospira, Inc. Formulations of low dose diclofenac and beta-cyclodextrin

Citations (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5275824A (en) * 1990-03-06 1994-01-04 Vectorpharma International Spa Therapeutic compositions with controlled release of medicaments supported on crosslinked polymers and coated with polymer films, and their preparation process
US5399584A (en) * 1992-05-05 1995-03-21 The Procter & Gamble Company Use of flavone derivatives for gastroprotection
US5788987A (en) * 1997-01-29 1998-08-04 Poli Industria Chimica Spa Methods for treating early morning pathologies
US5993860A (en) * 1993-06-17 1999-11-30 Venture Lending NSADI delivery employing a powdered hydrocolloid gum obtainable from higher plants
US6066643A (en) * 1997-10-17 2000-05-23 Eli Lilly And Company Potentiation of pharmaceuticals

Patent Citations (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5275824A (en) * 1990-03-06 1994-01-04 Vectorpharma International Spa Therapeutic compositions with controlled release of medicaments supported on crosslinked polymers and coated with polymer films, and their preparation process
US5399584A (en) * 1992-05-05 1995-03-21 The Procter & Gamble Company Use of flavone derivatives for gastroprotection
US5993860A (en) * 1993-06-17 1999-11-30 Venture Lending NSADI delivery employing a powdered hydrocolloid gum obtainable from higher plants
US5788987A (en) * 1997-01-29 1998-08-04 Poli Industria Chimica Spa Methods for treating early morning pathologies
US6066643A (en) * 1997-10-17 2000-05-23 Eli Lilly And Company Potentiation of pharmaceuticals

Cited By (10)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
EP1465601A2 (en) * 2001-12-28 2004-10-13 Teva Pharmaceutical Industries Ltd. A stable pharmaceutical formulation of paroxetine hydrochloride anhydrous and a process for preparation thereof
EP1465601A4 (en) * 2001-12-28 2006-02-15 Teva Pharma A stable pharmaceutical formulation of paroxetine hydrochloride anhydrous and a process for preparation thereof
US7396542B2 (en) 2001-12-28 2008-07-08 Teva Pharmaceutical Industries Ltd. Stable pharmaceutical formulation of paroxetine hydrochloride anhydrous and a process for preparation thereof
WO2006119779A2 (en) * 2005-05-10 2006-11-16 Lifecycle Pharma A/S A pharmaceutical composition comprising an aldosterone antagonist in form of solid solution
WO2006119779A3 (en) * 2005-05-10 2007-06-14 Lifecycle Pharma As A pharmaceutical composition comprising an aldosterone antagonist in form of solid solution
US8580954B2 (en) 2006-03-28 2013-11-12 Hospira, Inc. Formulations of low dose diclofenac and beta-cyclodextrin
US8946292B2 (en) 2006-03-28 2015-02-03 Javelin Pharmaceuticals, Inc. Formulations of low dose diclofenac and beta-cyclodextrin
WO2011130500A1 (en) * 2010-04-16 2011-10-20 Novartis Ag Formulations of a pyridazine bipyrazinyl
WO2011133675A1 (en) * 2010-04-21 2011-10-27 Teva Pharmaceutical Industries Ltd. Gabapentin enacarbil compositions
US20110263701A1 (en) * 2010-04-21 2011-10-27 Sigal Blau Gabapentin enacarbil compositions

Also Published As

Publication number Publication date
AU5152900A (en) 2000-12-12
EP1185251A1 (en) 2002-03-13

Similar Documents

Publication Publication Date Title
CA1146866A (en) Process for the production of sustained release pharmaceutical composition of solid medical material
FI87424C (en) Process for the preparation of solid nifedipine preparations which are readily biodegradable and which have a delayed effect
US5015479A (en) Sustained release capsule or tablet formulation comprising a pharmaceutically acceptable dihydropyridine
US6497905B1 (en) Aqueous solubility pharmaceutical formulations
JP3233638B2 (en) Method for producing freeze-dried drug dosage forms
CN1146419C (en) Formulation of fast-dissolving efavirenz capsules or tablets using super-disintegrants
US5972381A (en) Solid solution of an antifungal agent with enhanced bioavailability
RU2497502C2 (en) New method for preparing dry water-dispersed pharmaceutical forms, and pharmaceutical compositions prepared by such method
BG64368B1 (en) Pharmaceutical itraconazole compositions
IE63321B1 (en) Drug delivery system
WO2002034254A1 (en) Nateglinide-containing preparations
TW200835524A (en) Solid dispersion composition
TWI380829B (en) Solid dispersion composition of pranlukast with improved bioavailibility and the method of preparing the solid dispersion
IE59540B1 (en) Sustained release capsule or tablet formulation
EP0954288B1 (en) Solid solution of an antifungal agent with enhanced bioavailability
EP2242483A1 (en) Raloxifene composition
EP1929997A1 (en) Oxcarbazepine formulations
EP1185251A1 (en) A pharmaceutical composition containing an active agent that is maintained in solid amorphous form and method of making the same
JPH08291063A (en) Readily absorbable pharmaceutical preparation and its production
EP0996449A1 (en) Pharmaceutical compositions comprising cefuroxime axetil
WO2007075171A1 (en) Pharmaceutical formulations of fenofibrate having improved bioavailability
KR102594715B1 (en) Solid dispersion comprising niclosamide with increased oral bioavailability and preparation method thereof
CA2253769C (en) Pharmaceutical compositions comprising fenofibrate
WO2007141806A1 (en) Pharmaceutical formulations comprising oxcarbazepine and methods thereof
WO2009034409A2 (en) Pharmaceutical compositions of rhein or diacerein

Legal Events

Date Code Title Description
AK Designated states

Kind code of ref document: A1

Designated state(s): AE AG AL AM AT AU AZ BA BB BG BR BY CA CH CN CR CU CZ DE DK DM DZ EE ES FI GB GD GE GH GM HR HU ID IL IN IS JP KE KG KP KR KZ LC LK LR LS LT LU LV MA MD MG MK MN MW MX MZ NO NZ PL PT RO RU SD SE SG SI SK SL TJ TM TR TT TZ UA UG UZ VN YU ZA ZW

AL Designated countries for regional patents

Kind code of ref document: A1

Designated state(s): GH GM KE LS MW MZ SD SL SZ TZ UG ZW AM AZ BY KG KZ MD RU TJ TM AT BE CH CY DE DK ES FI FR GB GR IE IT LU MC NL PT SE BF BJ CF CG CI CM GA GN GW ML MR NE SN TD TG

121 Ep: the epo has been informed by wipo that ep was designated in this application
DFPE Request for preliminary examination filed prior to expiration of 19th month from priority date (pct application filed before 20040101)
WWE Wipo information: entry into national phase

Ref document number: 2000936175

Country of ref document: EP

WWP Wipo information: published in national office

Ref document number: 2000936175

Country of ref document: EP

REG Reference to national code

Ref country code: DE

Ref legal event code: 8642

WWW Wipo information: withdrawn in national office

Ref document number: 2000936175

Country of ref document: EP

NENP Non-entry into the national phase

Ref country code: JP