WO2017106214A1 - Amorphous onapristone compositions and methods of making the same - Google Patents

Amorphous onapristone compositions and methods of making the same Download PDF

Info

Publication number
WO2017106214A1
WO2017106214A1 PCT/US2016/066420 US2016066420W WO2017106214A1 WO 2017106214 A1 WO2017106214 A1 WO 2017106214A1 US 2016066420 W US2016066420 W US 2016066420W WO 2017106214 A1 WO2017106214 A1 WO 2017106214A1
Authority
WO
WIPO (PCT)
Prior art keywords
onapristone
amorphous
composition
polyethylene glycol
mixture
Prior art date
Application number
PCT/US2016/066420
Other languages
French (fr)
Inventor
Harry G. Brittain
Stefan PRONIUK
Original Assignee
Arno Therapeutics, Inc.
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 Arno Therapeutics, Inc. filed Critical Arno Therapeutics, Inc.
Priority to MX2018007154A priority Critical patent/MX2018007154A/en
Priority to CA3008422A priority patent/CA3008422A1/en
Priority to AU2016370499A priority patent/AU2016370499B2/en
Priority to EP16876503.0A priority patent/EP3389632A4/en
Priority to CN201680077010.2A priority patent/CN108883067B/en
Priority to JP2018532190A priority patent/JP2019503353A/en
Priority to KR1020187019175A priority patent/KR20180113988A/en
Publication of WO2017106214A1 publication Critical patent/WO2017106214A1/en
Priority to HK18114258.8A priority patent/HK1255104A1/en
Priority to HK18115767.9A priority patent/HK1256633A1/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
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K31/00Medicinal preparations containing organic active ingredients
    • A61K31/56Compounds containing cyclopenta[a]hydrophenanthrene ring systems; Derivatives thereof, e.g. steroids
    • A61K31/575Compounds containing cyclopenta[a]hydrophenanthrene ring systems; Derivatives thereof, e.g. steroids substituted in position 17 beta by a chain of three or more carbon atoms, e.g. cholane, cholestane, ergosterol, sitosterol
    • 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
    • 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
    • A61K9/1629Organic macromolecular compounds
    • A61K9/1635Organic macromolecular compounds obtained by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyvinyl pyrrolidone, poly(meth)acrylates
    • 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
    • A61K9/1629Organic macromolecular compounds
    • A61K9/1641Organic macromolecular compounds obtained otherwise than by reactions only involving carbon-to-carbon unsaturated bonds, e.g. polyethylene glycol, poloxamers
    • 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
    • A61K9/1682Processes
    • 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
    • A61K9/1682Processes
    • A61K9/1694Processes resulting in granules or microspheres of the matrix type containing more than 5% of excipient
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P5/00Drugs for disorders of the endocrine system
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07JSTEROIDS
    • C07J41/00Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring
    • C07J41/0033Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring not covered by C07J41/0005
    • C07J41/0055Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring not covered by C07J41/0005 the 17-beta position being substituted by an uninterrupted chain of at least three carbon atoms which may or may not be branched, e.g. cholane or cholestane derivatives, optionally cyclised, e.g. 17-beta-phenyl or 17-beta-furyl derivatives
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07JSTEROIDS
    • C07J41/00Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring
    • C07J41/0033Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring not covered by C07J41/0005
    • C07J41/0077Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring not covered by C07J41/0005 substituted in position 11-beta by a carbon atom, further substituted by a group comprising at least one further carbon atom
    • C07J41/0083Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring not covered by C07J41/0005 substituted in position 11-beta by a carbon atom, further substituted by a group comprising at least one further carbon atom substituted in position 11-beta by an optionally substituted phenyl group not further condensed with other rings
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07BGENERAL METHODS OF ORGANIC CHEMISTRY; APPARATUS THEREFOR
    • C07B2200/00Indexing scheme relating to specific properties of organic compounds
    • C07B2200/13Crystalline forms, e.g. polymorphs

Definitions

  • Onapristone ((8S, l lR,13R,14S, 17S)-l l-[4-(dimethylamino)phenyl]- 17-hydroxy-17-(3-hydroxypropyl)-13-methyl-l,2,6,7,8,l l, 12,14,15,16- decahydrocyclopenta[a]phenanthren-3-one) is an anti -progestin drug and progesterone receptor antagonist has the following structure:
  • Onapristone is known to be an amorphous compound.
  • Onapristone has previously been isolated as an amorphous solid and as a yellow oil.
  • (3-Acyloxypropyl)-derivatives of onapristone were identified as crystalline. See, U.S. Patent Number 4,780,461.
  • Recently, however, crystalline forms of onapristone have been identified. See, e ⁇ , U.S. Patent Publication Number 2014/0271819.
  • amorphous refers to the non-crystalline form of a chemical compound. Whereas the crystalline forms of a compound are characterized by structures assembled by the repetitive building up of fundamental units containing the molecules of the compound (known as unit cells), amorphous compounds have no such long-range repetitive structure, and are characterized by short-range, random ordering. Consequently, the lack of crystalline structure inherent to an amorphous compound may lead to significant differences in the physical and chemical properties of the compound, such as its solubility, dissolution rate, stability, bioavailability, and efficacy.
  • the amorphous form of a drug substance can be compared to crystalline forms of the compound using by a variety of techniques including, but not limited, to melting point, thermogravimetric analysis (TGA), differential scanning calorimetry (DSC), X-ray powder diffraction (XRPD), high performance liquid chromatography (HPLC), Raman microscopy, FT-IR spectroscopy, and solid-state nuclear magnetic resonance (ssNMR).
  • TGA thermogravimetric analysis
  • DSC differential scanning calorimetry
  • XRPD X-ray powder diffraction
  • HPLC high performance liquid chromatography
  • Raman microscopy FT-IR spectroscopy
  • solid-state nuclear magnetic resonance ssNMR
  • co-precipitate refers to the simultaneous precipitation of more than one compound together in a single-phase solid form from a solution.
  • Precipitate refers to the formation of a solid from a liquid solution. Precipitates can be used, for example, to modulate the properties of a chemical compound (e.g.,
  • aspects disclosed herein provide amorphous onapristone compositions and methods of making amorphous onapristone including, for example, by (1) pH cycling, (2) solvation-desolvation, (3) spray-drying onapristone/polymer mixtures, (4) solution- coprecipitation, and (4) solidification of hot melts.
  • One aspect provides methods of making amorphous onapristone by "pH cycling".
  • onapristone bulk drug substance is dissolved in a solvent, decreasing the pH of the resulting solution to dissolve the compound, and subsequently increasing the pH of the resulting solution to form an amorphous precipitate.
  • Another aspect provides methods of making amorphous onapnstone by dissolving onapnstone in a suitable solvent, followed by evaporation of the solution to yield a solvate, and then desolvating the solvate under controlled conditions to yield amorphous drug substance.
  • compositions comprising amorphous onapristone and polymeric excipients. These compositions may be obtained, for example, spray-drying or precipitation from a solution.
  • Yet another aspect provides methods of making amorphous onapristone by a "hot melt” process, whereby onapristone and various polymers are heated to form a polymer melt where the onapristone is dissolved in the resulting mixture. The melt is subsequently cooled to obtain the composition.
  • Compositions comprising onapristone and various polymers are also provided.
  • amorphous onapristone can be prepared as a pure drug substance, either through the use of a pH-cycling method or by controlled desolvation of the methanol solvate of onapristone.
  • the pH-cycled product remains amorphous for extended periods of time. For example, the pH-cycled product has been shown to remain amorphous for at least 16.5 months, while the solvation-desolvation product was shown to remain amorphous for at least 29 weeks (i.e., 7.25 months).
  • onapristone When spray-dried along with appropriate polymeric excipients, onapristone can be obtained in the form of an amorphous dispersion at a 25% w/w drug loading level. Two such dispersions have been shown to remain amorphous for at least 15 months.
  • onapristone When processed using a hot-melt procedure together with appropriate polymeric excipients, onapristone can be obtained in the form of an amorphous dispersion at a nominal 25% w/w drug loading level. Seven such dispersions have been shown to remain amorphous for at least 8 weeks (i.e., two months). [0016] Amorphous onapristone compositions as described herein, and made according to methods described herein, are stable in their amorphous state and retain their amorphous properties when stored under ambient conditions.
  • Figure 1 shows exemplary X-ray powder diffraction patterns of onapristone produced by the pH-cycle method
  • Figure 2 shows exemplary X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing polyvinyl pyrrolidone VA64) produced by the spray- drying method, and stored for various time periods;
  • Figure 3 shows exemplary X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing hydroxypropyl methylcellulose succinate M) produced by the spray-drying method, and stored for various time periods;
  • Figure 4 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing Kollidon®® 30 (polyvinylpyrrolidone)) produced by the hot-melt method, and stored for various time periods;
  • Figure 5 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing polyvinyl pyrrolidone K29/32) produced by the hot-melt method, and stored for various time periods ;
  • Figure 6 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing polyethylene glycol 8000) produced by the hot-melt method, and stored for various time periods;
  • Figure 7 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods;
  • Figure 8 shows exemplary X-ray powder diffraction patterns of approximately 25%) w/w onapristone dispersions (containing 27.1% w/w polyvinyl pyrrolidone K29/32 and 72.9%o w/w polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods;
  • Figure 9 shows exemplary X-ray powder diffraction patterns of approximately 25% w/w onapristone dispersions (containing 49.3% w/w polyvinyl pyrrolidone K29/32 and 50.7% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods;
  • Figure 10 shows exemplary X-ray powder diffraction patterns of approximately 25%) w/w onapristone dispersions (containing 73.5% w/w polyvinyl pyrrolidone K29/32 and 26.5%) w/w polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods;
  • Figure 11 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing Kollidon® 30 produced by the solution-phase coprecipitate method, prepared to contain varying amounts of onapristone;
  • Figure 12 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing polyvinylpyrrolidone K29/32 produced by the solution- phase coprecipitate method, prepared to contain varying amounts of onapristone;
  • Figure 13 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing polyethylene glycol 3350 produced by the solution-phase coprecipitate method, prepared to contain varying amounts of onapristone;
  • Figure 14 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing polyethylene glycol 8000 produced by the solution-phase coprecipitate method, prepared to contain varying amounts of onapristone;
  • Figure 15 shows exemplary X-ray powder diffraction patterns of
  • aspects described herein provide amorphous forms of onapristone which have advantageous properties including but not limited to increased bioavailability, increased stability, increased dissolution rate, and increased solubility. In one aspect, these properties relate to properties that will impart advantages with respect to formulating onapristone into a suitable dosage form.
  • Amorphous forms of onapristone have varying physical and chemical properties with respect, for example, solubility, melting temperature, and hygroscopicity, which may affect the stability of a particular dosage form of onapristone.
  • Drug formulation and dosage form selection have a significant impact on the cost of manufacturing.
  • Physical properties such as flow, particle size, surface area, and hardness may significantly impact the pharmacokinetics of the drug. For example, the dissolution and subsequent absorption of the drug in the body will affect the maximum concentration in the blood, clearance of the drug, and whether the drug is resident in the body for the optimal period of time.
  • amorphous onapristone is formed by adding onapristone to water, dissolving the onapristone in the water by adding one equivalent of an acid solution, and subsequently increasing the pH of the solution by the addition of one equivalent of base. At the end of this process, an amorphous precipitate is formed which may be isolated and characterized.
  • the XPRD pattern of the precipitated onapristone does not produce any substantially sharp scattering peaks.
  • the presence of a crystalline substance is indicated by the presence of sharp peaks (i.e., those whose width at half-height is in the range of 0.3 to 0.5 degrees 2 ⁇ ) in an XRPD pattern, while the XRPD pattern of an amorphous substance is characterized by the presence of broad scattering peaks (i.e., those whose width at half-height is in the range of at least 8 to 12 degrees 2 ⁇ ).
  • the acid solution comprises any suitable acid (e.g., hydrochloric acid (HC1), nitric acid (HNCb), or sulfuric acid (H2SO4)).
  • the acid is hydrochloric acid.
  • the base is any suitable base (e.g., sodium hydroxide (NaOH), potassium hydroxide (KOH), or ammonium hydroxide (NH4OH)).
  • the base is sodium hydroxide.
  • onapristone is first dissolved in methanol, and the resulting solution allowed to dry yielding an onapri stone/methanol solvate. If this resulting solvated form is heated at a temperature sufficient to desolvate the solid (e.g., around 100°C) for the minimal amount of time (e.g., less than 10 minutes), amorphous onapristone is formed.
  • compositions comprising onapristone (25%) in a polyvinylpyrrolidone VA64 copolymer matrix (i.e., onapri stone/P VP VA 64).
  • aspects provide methods of spray drying amorphous onapristone by spray drying onapri stone/P VP VA 64 from a solution comprising about 8% w/w solids in methanol resulting in amorphous onapristone.
  • compositions comprising onapristone and Kollidon® (polyvinylpyrrollidone) 30 (onapristone/Kollidon® 30).
  • onapristone and Kollidon® polyvinylpyrrollidone
  • onapristone/Kollidon® 30 onapristone/Kollidon® 30.
  • composition comprises about 0.255 g of onapristone and about 0.777 g of Kollidon® 30.
  • Another aspect provides methods of making amorphous onapristone by heating onapristone/Kollidon® 30 until the Kollidon® 30 melts, forming a molten mixture wherein the onapristone is dissolved in the polymer melt. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone.
  • the onapristone content of the glassy solid is about 24% w/w.
  • compositions comprising onapristone and
  • polyethylene glycol 8000 (Onapristone/Kollidon® 30).
  • composition comprises about 0.241 g of onapristone and about 0.700 g of polyethylene glycol 8000.
  • Further aspects provide methods of making amorphous onapristone by heating onapri stone/polyethylene glycol 8000 until the polyethylene glycol 8000 melts forming a polymer melt, and the onapri stone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone.
  • the onapristone content of the glassy solid is about 25% w/w.
  • compositions comprising onapristone and
  • polyethylene glycol 3350 (onapristone/polyethylene glycol 3350).
  • the composition comprises about 0.238 g of onapristone and about 0.762 g of polyethylene glycol 3350.
  • Further aspects provide methods of making amorphous onapristone by heating onapristone/ polyethylene glycol 3350 until the polyethylene glycol 3350 melts forming a polymer melt, and the onapristone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone.
  • the onapristone content of the glassy solid is about 23% w/w.
  • compositions comprising onapristone and
  • the composition comprises about 0.249 g of onapristone and about 0.784 g of pyrrolidone K29/32.
  • Further aspects provide methods of making amorphous onapristone by heating onapristone/pyrrolidone K29/32 until the pyrrolidone K29/32 melts forming a polymer melt, and the onapristone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone.
  • the onapristone content of the glassy solid is about 24% w/w.
  • compositions comprising onapristone, polyvinyl pyrrolidone K29/32, and polyethylene glycol 3350 (onapristone/pyrrolidone
  • the composition comprises about 0.258 g of
  • the composition comprises about 0.242 g of onapristone, about 0.373 g of polyvinyl pyrrolidone K29/32, and about 0.384 g of polyethylene glycol 3350. In yet another aspect, the composition comprises about 0.241 g of onapristone, about 0.547 g of polyvinyl pyrrolidone K29/32, and about 0.197 g of polyethylene glycol 3350.
  • Further aspects provide methods of making amorphous onapristone by heating onapristone/pyrrolidone K29/32 until the polyvinyl pyrrolidone K29/32 and polyethylene glycol 3350 melts forming a polymer melt, and the onapristone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone.
  • Figure 1 shows X-ray powder diffraction patterns of onapristone as initially produced by the pH-cycle method, and stored under ambient conditions for 25 weeks, 43 weeks, and 16.5 months.
  • Figure 2 shows X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing polyvinyl pyrrolidone VA64) produced by the spray-drying method, and stored under ambient conditions for 12 weeks, 20 weeks, 36 weeks, and 15 months.
  • Figure 3 shows X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing hydroxypropyl methylcellulose succinate M) produced by the spray- drying method, and stored under ambient conditions for 12 weeks, 20 weeks, 36 weeks, and 15 months.
  • Figure 4 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing Kollidon® 30) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
  • Figure 5 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing polyvinyl pyrrolidone K29/32) produced by the hot- melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
  • Figure 6 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing polyethylene glycol 8000) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
  • the XRPD pattern for polyethylene glycol 8000 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
  • Figure 7 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
  • the XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
  • Figure 8 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing 27.1% w/w polyvinyl pyrrolidone K29/32 and 72.9% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
  • the XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
  • Figure 9 shows X-ray powder diffraction patterns of nominal 25%) w/w onapristone dispersions (containing 49.3% w/w polyvinyl pyrrolidone K29/32 and 50.7% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
  • the XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
  • Figure 10 shows X-ray powder diffraction patterns of nominal 25%) w/w onapristone dispersions (containing 73.5% w/w polyvinyl pyrrolidone K29/32 and 26.5% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
  • the XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
  • Figure 11 shows X-ray powder diffraction patterns of onapristone dispersions containing Kollidon® 30 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for Kollidon® 30 itself is shown for comparison purposes.
  • Figure 12 shows X-ray powder diffraction patterns of onapristone dispersions containing polyvinylpyrrolidone K29/32 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for polyvinylpyrrolidone K29/32 itself is shown for comparison purposes.
  • Figure 13 shows X-ray powder diffraction patterns of onapristone dispersions containing polyethylene glycol 3350 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes (demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient).
  • Figure 14 shows X-ray powder diffraction patterns of onapristone dispersions containing polyethylene glycol 8000 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for polyethylene glycol 8000 itself is shown for comparison purposes (demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient).
  • Figure 15 shows X-ray powder diffraction patterns of nominal 25% onapristone dispersions containing various amounts of Kollidon® 30 and polyethylene glycol 8000 produced by the solution-phase coprecipitate method. The relative percentages of the two polymers are indicated.
  • the onapristone amorphous forms can be used to treat a patient in need of treatment as described herein.
  • the terms "treat,” “prevent,” or similar terms, as used herein, do not necessarily mean 100% or complete treatment or prevention. Rather, these terms refer to various degrees of treatment or prevention of a particular disease (e.g., 100%, 90%, 80%, 70%, 60%, 50%, 40%, 30%, 20%, 10%, 5%, or 1%) as recognized in the art as being beneficial.
  • treatment or “prevention” also refer to delaying onset of a disease for a period of time or delaying onset indefinitely.
  • treatment refers to administering a drug or treatment to a patient or prescribing a drug to a patient where the patient or a third party (e.g., caretaker, family member, or health care professional) administers the drug or treatment.
  • a third party e.g., caretaker, family member, or health care professional
  • the onapristone amorphous forms also encompass derivatives.
  • the term “derivative” includes, but is not limited to, ether derivatives, acid derivatives, amide derivatives, ester derivatives and the like. Methods of preparing these derivatives are known to a person skilled in the art. For example, ether derivatives are prepared by the coupling of the corresponding alcohols. Amide and ester derivatives are prepared from the corresponding carboxylic acid by a reaction with amines and alcohols, respectively.
  • the onapristone amorphous forms also encompass hydrates or solvates of onapristone amorphous or crystalline forms (e.g., hemihydrate, monohydrate, dihydrate, trihydrate and the like). Hydrates or solvates of onapristone may be prepared by contacting onapristone with water or a solvent under suitable conditions to produce the hydrate or solvate of choice, for example, as described herein.
  • the onapristone amorphous forms also encompass metabolites of onapristone amorphous forms.
  • Metabolite or “metabolites” refer to any substance produced from another substance by metabolism or a through a metabolic process of a living cell or organ.
  • the onapristone amorphous compounds can be formulated into suitable pharmaceutical preparations such as tablets, capsules, or elixirs for oral administration or in sterile solutions or suspensions for parenteral administration.
  • suitable pharmaceutical preparations such as tablets, capsules, or elixirs for oral administration or in sterile solutions or suspensions for parenteral administration.
  • the onapristone amorphous compounds described herein can be formulated into pharmaceutical compositions using techniques and procedures well known in the art.
  • about 10 to about 200 mg of the onapristone amorphous compounds, or a physiologically acceptable salt, pro-drug, or co-crystal thereof can be compounded or used as a starting material for compounding with a physiologically acceptable vehicle, carrier, excipient, binder, preservative, stabilizer, flavor, etc., in a unit dosage form as called for by accepted pharmaceutical practice.
  • the amount of active substance in compositions or preparations comprising the onapristone amorphous compounds is such that a suitable dosage in the range indicated is obtained.
  • compositions can be formulated in a unit dosage form, each dosage containing from about 1 mg to about 1.2 g, or about 2.5 to about 200 mg of the active ingredient.
  • unit dosage from refers to physically discrete units suitable as unitary dosages for human subjects and other mammals, each unit containing a predetermined quantity of active material calculated to produce the desired therapeutic effect, in association with one or more suitable pharmaceutical excipients.
  • one or more of the onapristone amorphous compounds are mixed with or used as starting materials mixed with a suitable pharmaceutically acceptable carrier to form compositions.
  • the resulting mixture may be a solution, suspension, emulsion, or the like.
  • Liposomal suspensions may also be used as pharmaceutically acceptable carriers. These may be prepared according to methods known to those skilled in the art.
  • the form of the resulting mixture depends upon a number of factors, including the intended mode of administration and the solubility of the compound in the selected carrier or vehicle.
  • the effective concentration is sufficient for lessening or ameliorating at least one symptom of the disease, disorder, or condition treated and may be empirically determined.
  • Pharmaceutical carriers or vehicles suitable for administration of the onapristone amorphous compounds described herein include any such carriers suitable for the particular mode of administration.
  • the active materials can also be mixed with other active materials that do not impair the desired action, or with materials that supplement the desired action, or have another action.
  • the compounds may be formulated as the sole pharmaceutically active ingredient in the composition or may be combined with other active ingredients.
  • DMSO dimethylsulfoxide
  • TWEEN surfactants
  • dissolution in aqueous sodium bicarbonate aqueous sodium bicarbonate.
  • Derivatives of the compounds, such as salts or prodrugs, may also be used in formulating effective pharmaceutical compositions.
  • the concentration of the compound is effective for delivery of an amount upon administration that lessens or ameliorates at least one symptom of the disorder for which the compound is administered.
  • the compositions are formulated for single dosage administration.
  • the onapristone amorphous compounds described herein may be prepared with carriers that protect them against rapid elimination from the body, such as time-release formulations or coatings.
  • Such carriers include controlled release formulations, such as, but not limited to, microencapsulated delivery systems.
  • the active compound can be included in the pharmaceutically acceptable carrier in an amount sufficient to exert a therapeutically useful effect in the absence of undesirable side effects on the patient treated.
  • the therapeutically effective concentration may be determined empirically by testing the compounds in known in vitro and in vivo model systems for the treated disorder.
  • the onapristone amorphous compounds and compositions described herein can be enclosed in multiple or single dose containers.
  • the enclosed compounds and compositions can be provided in kits, for example, including component parts that can be assembled for use.
  • an onapristone amorphous compound can be used as a starting material for a lyophilized form and a suitable diluent may be provided as a separated component for combination prior to use.
  • a kit may include onapristone amorphous compound and a second therapeutic agent for co-administration.
  • the onapristone amorphous compound and second therapeutic agent may be provided as separate component parts.
  • a kit may include a plurality of containers, each container holding one or more unit dose of the onapristone amorphous compounds described herein.
  • the containers can be adapted for the desired mode of
  • composition will depend on dissolution, absorption, metabolism, and excretion rates of the active compound, the dosage schedule, and amount administered as well as other factors known to those of skill in the art.
  • the active ingredient may be administered at once, or may be divided into a number of smaller doses to be administered at intervals of time. It is understood that the precise dosage and duration of treatment is a function of the disease being treated and may be determined empirically using known testing protocols or by extrapolation from in vivo or in vitro test data. It is to be noted that concentrations and dosage values may also vary with the severity of the condition to be alleviated. It is to be further understood that for any particular subject, specific dosage regimens should be adjusted over time according to the individual need and the professional judgment of the person administering or supervising the administration of the compositions, and that the concentration ranges set forth herein are exemplary only and are not intended to limit the scope or practice of the claimed compositions.
  • the compound can be provided in a composition that protects it from the acidic environment of the stomach.
  • the composition can be formulated in an enteric coating that maintains its integrity in the stomach and releases the active compound in the intestine.
  • the composition may also be formulated in combination with an antacid or other such ingredient.
  • Oral compositions will generally include an inert diluent or an edible carrier and may be compressed into tablets or enclosed in gelatin capsules.
  • the active compound or compounds can be incorporated with excipients and used in the form of tablets, capsules, or troches.
  • Pharmaceutically compatible binding agents and adjuvant materials can be included as part of the composition.
  • the tablets, pills, capsules, troches, and the like can contain any of the following ingredients or compounds of a similar nature: a binder such as, but not limited to, gum tragacanth, acacia, corn starch, or gelatin; an excipient such as microcrystalline cellulose, starch, or lactose; a disintegrating agent such as, but not limited to, alginic acid and corn starch; a lubricant such as, but not limited to, magnesium stearate; a glidant, such as, but not limited to, colloidal silicon dioxide; a sweetening agent such as sucrose or saccharin; and a flavoring agent such as peppermint, methyl salicylate, or fruit flavoring.
  • a binder such as, but not limited to, gum tragacanth, acacia, corn starch, or gelatin
  • an excipient such as microcrystalline cellulose, starch, or lactose
  • a disintegrating agent such as, but not limited to, algin
  • the dosage unit form when it is a capsule, it can contain, in addition to material of the above type, a liquid carrier such as a fatty oil.
  • dosage unit forms can contain various other materials, which modify the physical form of the dosage unit, for example, coatings of sugar and other enteric agents.
  • the compounds can also be administered as a component of an elixir, suspension, syrup, wafer, chewing gum or the like.
  • a syrup may contain, in addition to the active compounds, sucrose as a sweetening agent and certain preservatives, dyes and colorings, and flavors.
  • the active materials can also be mixed with other active materials that do not impair the desired action, or with materials that supplement the desired action.
  • the onapristone amorphous compounds can be used, for example, in combination with an antitumor agent, a hormone, a steroid, or a retinoid.
  • the antitumor agent may be one of numerous chemotherapy agents (e.g., everolimus, trastuzumab, TM1-D, anti-HER2 drugs, bevacizumab, paclitaxel, docetaxel, taxanes, doxorubicin, liposomal doxorubicin, pegylated liposomal doxorubicin, anthracyclines, anthracenediones, carboplatin, cisplatin, 5-FU, gemcitabine and cyclophosphamide).
  • chemotherapy agents e.g., everolimus, trastuzumab, TM1-D, anti-HER2 drugs, bevacizumab, paclitaxel, docetaxel, taxanes, doxorubicin, liposomal doxorubicin, pegylated liposomal doxorubicin, anthracyclines, anthracenediones, carboplatin, cisplatin
  • solutions or suspensions used for parenteral, intradermal, subcutaneous, or topical application can include any of the following components: a sterile diluent such as water for injection, saline solution, fixed oil, a naturally occurring vegetable oil such as sesame oil, coconut oil, peanut oil, cottonseed oil, and the like, or a synthetic fatty vehicle such as ethyl oleate, and the like, polyethylene glycol, glycerin, propylene glycol, or other synthetic solvent; antimicrobial agents such as benzyl alcohol and methyl parabens; antioxidants such as ascorbic acid and sodium bisulfite; chelating agents such as ethylenediaminetetraacetic acid (EDTA) or its disodium salt; buffers such as acetates, citrates, and phosphates; and agents for the adjustment of tonicity such as sodium chloride and dextrose.
  • a sterile diluent such as water for injection, saline solution, fixed oil
  • suitable carriers include, but are not limited to, physiological saline, phosphate buffered saline (PBS), and solutions containing thickening and solubilizing agents such as glucose, polyethylene glycol, polypropylene glycol, and mixtures thereof.
  • PBS phosphate buffered saline
  • suitable carriers include, but are not limited to, physiological saline, phosphate buffered saline (PBS), and solutions containing thickening and solubilizing agents such as glucose, polyethylene glycol, polypropylene glycol, and mixtures thereof.
  • Liposomal suspensions including tissue- targeted liposomes may also be suitable as pharmaceutically acceptable carriers. These may be prepared according to methods known in the art.
  • the onapristone amorphous compounds may be prepared with carriers that protect the compound against rapid elimination from the body, such as time-release formulations or coatings.
  • carriers include controlled release formulations, such as, but not limited to, implants and microencapsulated delivery systems, and biodegradable, biocompatible polymers such as collagen, ethylene vinyl acetate, polyanhydrides, polyglycolic acid, polyorthoesters, polylactic acid, hydroxyl propyl methyl cellulose (HPMC), other cellulose derivatives, and the like. Methods for preparation of such formulations are known to those skilled in the art.
  • compounds employed in the methods of the disclosure may be administered enterally or parenterally.
  • compounds employed in the methods of the disclosure can be administered in usual dosage forms for oral administration as is well known to those skilled in the art.
  • These dosage forms include the usual solid unit dosage forms of tablets and capsules as well as liquid dosage forms such as solutions, suspensions, and elixirs.
  • the solid dosage forms can be of the sustained release type so that the compounds employed in the methods described herein need to be administered only once or twice daily.
  • the oral dosage forms can be administered to the patient 1, 2, 3, or 4 times daily.
  • the onapristone amorphous compounds described herein can be administered either three or fewer times, or even once or twice daily.
  • the onapristone employed in the methods of the disclosure be administered in oral dosage form.
  • they can be designed so as to protect the compounds employed in the methods described herein from the acidic environment of the stomach. Enteric coated tablets are well known to those skilled in the art.
  • capsules filled with small spheres each coated to protect from the acidic stomach are also well known to those skilled in the art.
  • the terms "therapeutically effective amount” and “therapeutically effective period of time” are used to denote treatments at dosages and for periods of time effective to reduce neoplastic cell growth.
  • administration can be parenteral, oral, sublingual, transdermal, topical, intranasal, or intrarectal.
  • the therapeutic composition when administered systemically, can be administered at a sufficient dosage to attain a blood level of the compounds of from about 0.01 ⁇ to about 20 ⁇ . For localized administration, much lower concentrations than this can be effective, and much higher concentrations may be tolerated.
  • concentrations for localized administration, much lower concentrations than this can be effective, and much higher concentrations may be tolerated.
  • amorphous compound may vary considerably depending on the tissue, organ, or the particular animal or patient to be treated. It is also understood that while a patient may be started at one dose, that dose may be varied overtime as the patient's condition changes.
  • the onapri stone amorphous compounds can be used to inhibit the growth of tumors derived from tissue including, but not limited to, breast, brain, meningiomas, prostate, ovarian, endometrial, uterine leiomyoma, lung, and uterine tissues.
  • XRPD X-ray powder diffraction
  • XRPD patterns were obtained using a Rigaku MiniFlex powder diffraction system, equipped with a horizontal goniometer operating in the ⁇ /2 ⁇ mode.
  • the X-ray source was nickel-filtered Ka emission of copper (1.54184 A).
  • Samples were packed into the sample holder using a back-fill procedure, and were scanned over the range of 3.5 to 40 degrees 2 ⁇ at a scan rate of 0.5 degrees 29/min. Using a data acquisition rate of 1 point per second, these scanning parameters equate to a step size of 0.0084 degrees 2 ⁇ .
  • Calibration of the diffractometer system was effected using purified talc as a reference material. The intensity scale for all diffraction patterns was normalized so that the relative intensity of the most intense peak in the pattern equaled 100%.
  • the onapristone molecule contains a functional group that is effectively a substituted aniline:
  • this group In one aspect, one would expect this group to be somewhat acidic. Using the pKa-Predictor module of the Physical Chemistry Program Suite (Advanced Chemical Laboratories, Toronto, CA), the pKa of this group was predicted to be 5.30 ⁇ 0.25. Using the predictive solubility module of the ACD program, it was determined that the protonated form of the compound is expected to be fairly soluble in water, while the neutral form is expected to be relatively insoluble in water.
  • onapristone (0.91 mmol) was slurried in 25 mL of water, and then 0.5 mL of 2N HC1 (1.0 mmol) was added. The solid completely dissolved in approximately 5 minutes, whereupon 2.0 mL of 0.5 N NaOH (1.0 mmol) was added. The precipitated onapristone was suction-filtered, and allowed to air-dry overnight.
  • Sample ID SSF-PDS-027-001A comprising 25% onapristone in a matrix consisting of PVP VA64, and was spray-dried from a solution consisting of 8% w/w solids in methanol.
  • Sample ID SSF-PDS-027-001B comprising 25% onapristone in a matrix consisting of HPMCAS-M, and was spray-dried from a solution consisting of 8% w/w solids in methanol.
  • XRPD patterns of these samples were obtained when initially received and after 12 weeks, 20 weeks, 36 weeks, and 15 months had elapsed.
  • the XRPD patterns obtained for sample SSF-PDS-027-001A are collected in Figure 2, while the XRPD patterns obtained for sample SSF-PDS-027-001B are collected in Figure 3.
  • Preparation 2 0.241 g of onapristone and 0.700 g of polyethylene glycol 8000 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymer had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder.
  • the onapristone content of this sample was 25.6% w/w.
  • Preparation 3 0.238 g of onapristone and 0.762 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymer had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 23.8% w/w.
  • Preparation 4 0.249 g of onapristone and 0.784 g of polyvinyl pyrrolidone K29/32 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymer had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 24.1% w/w.
  • the XRPD pattern of formulations containing polyvinyl pyrrolidone are shown in Figures 4 and 5, respectively. Also shown in Figures 4 and 5 are the XRPD patterns of the same products after each had been stored under ambient conditions for time periods of 8 weeks and 8.5 months. Since no sharp peaks attributable to crystalline onapristone were detected in the XRPD of the preparations, it is concluded that the drug substance remained amorphous over the entire 8.5 month storage period.
  • the XRPD pattern of formulations containing polyethylene glycol are shown in Figures 6 and 7. Also shown in Figures 6 and 7 are the XRPD patterns of the same products after each had been stored under ambient conditions for time periods of 8-weeks and 8.5 months, as well as the XRPD patterns of the polyethylene glycol polymers used to form the products.
  • the XRPD patterns of the PEG polymer products are dominated by two scattering peaks at approximately 19 and 23 degrees 2 ⁇ . All of the polymer peaks were observed in the XRPD patterns of the dispersions, but no additional peaks attributable to crystalline onapristone were detected in the XRPD patterns of the preparations. Therefore, the drug substance remained amorphous over the entire 8.5 month storage period.
  • Preparation 5 0.258 g of onapristone, 0.202 g of polyvinyl pyrrolidone K29/32, and 0.543 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymers had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 25.7% w/w, and the PVP content in this sample was 27.1% w/w (relative to the total polymer concentration).
  • Preparation 6 0.242 g of onapristone, 0.373 g of polyvinyl pyrrolidone K29/32, and 0.384 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymers had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 24.2% w/w, and the PVP content in this sample was 49.3% w/w (relative to the total polymer concentration).
  • Preparation 7 0.241 g of onapristone, 0.547 g of polyvinyl pyrrolidone K29/32, and 0.197 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymers had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 24.5% w/w, and the PVP content in this sample was 73.5% w/w (relative to the total polymer concentration).
  • the XRPD patterns of these latter three preparations are shown in Figures 8-10, respectively, along with the XRPD patterns of the polyethylene glycol 3350 excipient. Also shown in Figures 8-10 are the XRPD patterns of the same products after each had been stored under ambient conditions for time periods of 8 weeks and 8.5 months.
  • the XRPD patterns of the hot-melt dispersions were dominated by the two scattering peaks (at approximately 19 and 23 degrees 2 ⁇ ) associated with the PEG-3350, but no additional peaks attributable to crystalline onapristone were detected in the XRPD of the preparations. Therefore, the drug substance remained amorphous over the 8 week storage period. In addition, all three dispersions were easily dislodged from the beaker, and their rendition into powder was straight-forward.
  • polyethylene glycol 3350 For preparations within the polyethylene glycol 3350 system, the requisite amount of onapristone and polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and 30 mL of absolute isopropanol was added to the beaker. The contents were heated and stirred until dissolution was complete, whereupon the solution was poured into an evaporating dish and allowed to completely air-dry.
  • the polyethylene glycol 3350 preparations had the following compositions:

Landscapes

  • Health & Medical Sciences (AREA)
  • Chemical & Material Sciences (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Engineering & Computer Science (AREA)
  • General Health & Medical Sciences (AREA)
  • Public Health (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Animal Behavior & Ethology (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Medicinal Chemistry (AREA)
  • Veterinary Medicine (AREA)
  • Epidemiology (AREA)
  • Organic Chemistry (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • Endocrinology (AREA)
  • General Chemical & Material Sciences (AREA)
  • Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
  • Diabetes (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Medicinal Preparation (AREA)
  • Analysing Materials By The Use Of Radiation (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)

Abstract

Amorphous forms of onapristone and methods of making such amorphous forms are provided. Amorphous forms can be characterized by their X-ray powder diffraction patterns and other properties.

Description

AMORPHOUS ONAPRISTONE COMPOSITIONS AND METHODS OF
MAKING THE SAME
PRIORITY CLAIM
[0001] This application claims priority to U.S. Provisional Patent Application Serial No. 62/267,540, filed December 15, 2015. The above referenced application is incorporated herein by reference as if restated in full.
[0002] All references cited herein, including but not limited to patents and patent applications, are incorporated by reference in their entirety.
BACKGROUND
[0003] Onapristone (ONA) ((8S, l lR,13R,14S, 17S)-l l-[4-(dimethylamino)phenyl]- 17-hydroxy-17-(3-hydroxypropyl)-13-methyl-l,2,6,7,8,l l, 12,14,15,16- decahydrocyclopenta[a]phenanthren-3-one) is an anti -progestin drug and progesterone receptor antagonist has the following structure:
Figure imgf000002_0001
[0004] Onapristone is known to be an amorphous compound. For example, Onapristone has previously been isolated as an amorphous solid and as a yellow oil. Neef, et al. Steroids, 1984, 44, 349; Neef, et al, DE3321826. In contrast to onapristone, (3-Acyloxypropyl)-derivatives of onapristone were identified as crystalline. See, U.S. Patent Number 4,780,461. Recently, however, crystalline forms of onapristone have been identified. See, e^, U.S. Patent Publication Number 2014/0271819. [0005] The term "amorphous," as used herein, refers to the non-crystalline form of a chemical compound. Whereas the crystalline forms of a compound are characterized by structures assembled by the repetitive building up of fundamental units containing the molecules of the compound (known as unit cells), amorphous compounds have no such long-range repetitive structure, and are characterized by short-range, random ordering. Consequently, the lack of crystalline structure inherent to an amorphous compound may lead to significant differences in the physical and chemical properties of the compound, such as its solubility, dissolution rate, stability, bioavailability, and efficacy.
[0006] The amorphous form of a drug substance can be compared to crystalline forms of the compound using by a variety of techniques including, but not limited, to melting point, thermogravimetric analysis (TGA), differential scanning calorimetry (DSC), X-ray powder diffraction (XRPD), high performance liquid chromatography (HPLC), Raman microscopy, FT-IR spectroscopy, and solid-state nuclear magnetic resonance (ssNMR). The physical stability of the amorphous form of a compound can be measured, for example, under conditions where the temperature and humidity in the environment are controlled for various time periods.
[0007] The term "co-precipitate" refers to the simultaneous precipitation of more than one compound together in a single-phase solid form from a solution. The term
"precipitate" refers to the formation of a solid from a liquid solution. Precipitates can be used, for example, to modulate the properties of a chemical compound (e.g.,
bioavailability, pharmacokinetics, stability).
SUMMARY
[0008] Aspects disclosed herein provide amorphous onapristone compositions and methods of making amorphous onapristone including, for example, by (1) pH cycling, (2) solvation-desolvation, (3) spray-drying onapristone/polymer mixtures, (4) solution- coprecipitation, and (4) solidification of hot melts.
[0009] One aspect provides methods of making amorphous onapristone by "pH cycling". In this procedure, onapristone bulk drug substance is dissolved in a solvent, decreasing the pH of the resulting solution to dissolve the compound, and subsequently increasing the pH of the resulting solution to form an amorphous precipitate.
[0010] Another aspect provides methods of making amorphous onapnstone by dissolving onapnstone in a suitable solvent, followed by evaporation of the solution to yield a solvate, and then desolvating the solvate under controlled conditions to yield amorphous drug substance.
[0011] Further aspects provide compositions comprising amorphous onapristone and polymeric excipients. These compositions may be obtained, for example, spray-drying or precipitation from a solution.
[0012] Yet another aspect provides methods of making amorphous onapristone by a "hot melt" process, whereby onapristone and various polymers are heated to form a polymer melt where the onapristone is dissolved in the resulting mixture. The melt is subsequently cooled to obtain the composition. Compositions comprising onapristone and various polymers are also provided.
[0013] As described herein, amorphous onapristone can be prepared as a pure drug substance, either through the use of a pH-cycling method or by controlled desolvation of the methanol solvate of onapristone. The pH-cycled product remains amorphous for extended periods of time. For example, the pH-cycled product has been shown to remain amorphous for at least 16.5 months, while the solvation-desolvation product was shown to remain amorphous for at least 29 weeks (i.e., 7.25 months).
[0014] When spray-dried along with appropriate polymeric excipients, onapristone can be obtained in the form of an amorphous dispersion at a 25% w/w drug loading level. Two such dispersions have been shown to remain amorphous for at least 15 months.
[0015] When processed using a hot-melt procedure together with appropriate polymeric excipients, onapristone can be obtained in the form of an amorphous dispersion at a nominal 25% w/w drug loading level. Seven such dispersions have been shown to remain amorphous for at least 8 weeks (i.e., two months). [0016] Amorphous onapristone compositions as described herein, and made according to methods described herein, are stable in their amorphous state and retain their amorphous properties when stored under ambient conditions.
FIGURES
[0017] Figure 1 shows exemplary X-ray powder diffraction patterns of onapristone produced by the pH-cycle method;
[0018] Figure 2 shows exemplary X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing polyvinyl pyrrolidone VA64) produced by the spray- drying method, and stored for various time periods;
[0019] Figure 3 shows exemplary X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing hydroxypropyl methylcellulose succinate M) produced by the spray-drying method, and stored for various time periods;
[0020] Figure 4 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing Kollidon®® 30 (polyvinylpyrrolidone)) produced by the hot-melt method, and stored for various time periods;
[0021] Figure 5 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing polyvinyl pyrrolidone K29/32) produced by the hot-melt method, and stored for various time periods ;
[0022] Figure 6 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing polyethylene glycol 8000) produced by the hot-melt method, and stored for various time periods;
[0023] Figure 7 shows exemplary X-ray powder diffraction patterns of approximately 25%o w/w onapristone dispersions (containing polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods;
[0024] Figure 8 shows exemplary X-ray powder diffraction patterns of approximately 25%) w/w onapristone dispersions (containing 27.1% w/w polyvinyl pyrrolidone K29/32 and 72.9%o w/w polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods; [0025] Figure 9 shows exemplary X-ray powder diffraction patterns of approximately 25% w/w onapristone dispersions (containing 49.3% w/w polyvinyl pyrrolidone K29/32 and 50.7% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods;
[0026] Figure 10 shows exemplary X-ray powder diffraction patterns of approximately 25%) w/w onapristone dispersions (containing 73.5% w/w polyvinyl pyrrolidone K29/32 and 26.5%) w/w polyethylene glycol 3350) produced by the hot-melt method, and stored for various time periods;
[0027] Figure 11 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing Kollidon® 30 produced by the solution-phase coprecipitate method, prepared to contain varying amounts of onapristone;
[0028] Figure 12 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing polyvinylpyrrolidone K29/32 produced by the solution- phase coprecipitate method, prepared to contain varying amounts of onapristone;
[0029] Figure 13 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing polyethylene glycol 3350 produced by the solution-phase coprecipitate method, prepared to contain varying amounts of onapristone;
[0030] Figure 14 shows exemplary X-ray powder diffraction patterns of binary onapristone dispersions containing polyethylene glycol 8000 produced by the solution-phase coprecipitate method, prepared to contain varying amounts of onapristone; and
[0031] Figure 15 shows exemplary X-ray powder diffraction patterns of
approximately 25% onapristone ternary dispersions containing various amounts of Kollidon® 30 and polyethylene glycol 8000 produced by the solution-phase coprecipitate method.
DETAILED DESCRIPTION
[0032] Before describing several exemplary aspects described herein, it is to be understood that the invention is not limited to the details of construction or process steps set forth in the following description and examples. The aspects described herein are capable of being practiced or being carried out in various ways. All publications, patents, and patent applications cited herein are incorporated by reference in their entirety.
[0033] Aspects described herein provide amorphous forms of onapristone which have advantageous properties including but not limited to increased bioavailability, increased stability, increased dissolution rate, and increased solubility. In one aspect, these properties relate to properties that will impart advantages with respect to formulating onapristone into a suitable dosage form.
[0034] Amorphous forms of onapristone have varying physical and chemical properties with respect, for example, solubility, melting temperature, and hygroscopicity, which may affect the stability of a particular dosage form of onapristone. Drug formulation and dosage form selection have a significant impact on the cost of manufacturing. Physical properties such as flow, particle size, surface area, and hardness may significantly impact the pharmacokinetics of the drug. For example, the dissolution and subsequent absorption of the drug in the body will affect the maximum concentration in the blood, clearance of the drug, and whether the drug is resident in the body for the optimal period of time.
[0035] In one aspect, amorphous onapristone is formed by adding onapristone to water, dissolving the onapristone in the water by adding one equivalent of an acid solution, and subsequently increasing the pH of the solution by the addition of one equivalent of base. At the end of this process, an amorphous precipitate is formed which may be isolated and characterized. In another aspect, the XPRD pattern of the precipitated onapristone does not produce any substantially sharp scattering peaks. The presence of a crystalline substance is indicated by the presence of sharp peaks (i.e., those whose width at half-height is in the range of 0.3 to 0.5 degrees 2Θ) in an XRPD pattern, while the XRPD pattern of an amorphous substance is characterized by the presence of broad scattering peaks (i.e., those whose width at half-height is in the range of at least 8 to 12 degrees 2Θ).
[0036] In one aspect, the acid solution comprises any suitable acid (e.g., hydrochloric acid (HC1), nitric acid (HNCb), or sulfuric acid (H2SO4)). In one aspect, the acid is hydrochloric acid. [0037] In another aspect, the base is any suitable base (e.g., sodium hydroxide (NaOH), potassium hydroxide (KOH), or ammonium hydroxide (NH4OH)). In one aspect, the base is sodium hydroxide.
[0038] In yet another aspect, the pH is reduced to pH=l or below. In a further aspect, when the pH is raised, it is increased to pH=10 or above.
[0039] In another aspect, onapristone is first dissolved in methanol, and the resulting solution allowed to dry yielding an onapri stone/methanol solvate. If this resulting solvated form is heated at a temperature sufficient to desolvate the solid (e.g., around 100°C) for the minimal amount of time (e.g., less than 10 minutes), amorphous onapristone is formed.
[0040] Yet another aspect provides compositions comprising onapristone (25%) in a polyvinylpyrrolidone VA64 copolymer matrix (i.e., onapri stone/P VP VA 64).
[0041] Aspects provide methods of spray drying amorphous onapristone by spray drying onapri stone/P VP VA 64 from a solution comprising about 8% w/w solids in methanol resulting in amorphous onapristone.
[0042] Another aspect provides compositions comprising onapristone and Kollidon® (polyvinylpyrrollidone) 30 (onapristone/Kollidon® 30). In another aspect, the
composition comprises about 0.255 g of onapristone and about 0.777 g of Kollidon® 30.
[0043] Another aspect provides methods of making amorphous onapristone by heating onapristone/Kollidon® 30 until the Kollidon® 30 melts, forming a molten mixture wherein the onapristone is dissolved in the polymer melt. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone. In another aspect, the onapristone content of the glassy solid is about 24% w/w.
[0044] Another aspect provides compositions comprising onapristone and
polyethylene glycol 8000 (Onapristone/Kollidon® 30). In another aspect, the
composition comprises about 0.241 g of onapristone and about 0.700 g of polyethylene glycol 8000.
[0045] Further aspects provide methods of making amorphous onapristone by heating onapri stone/polyethylene glycol 8000 until the polyethylene glycol 8000 melts forming a polymer melt, and the onapri stone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone. In another aspect, the onapristone content of the glassy solid is about 25% w/w.
[0046] Another aspect provides compositions comprising onapristone and
polyethylene glycol 3350 (onapristone/polyethylene glycol 3350). In another aspect, the composition comprises about 0.238 g of onapristone and about 0.762 g of polyethylene glycol 3350.
[0047] Further aspects provide methods of making amorphous onapristone by heating onapristone/ polyethylene glycol 3350 until the polyethylene glycol 3350 melts forming a polymer melt, and the onapristone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone. In another aspect, the onapristone content of the glassy solid is about 23% w/w.
[0048] Another aspect provides compositions comprising onapristone and
pyrrolidone K29/32 (onapristone/pyrrolidone K29/32). In another aspect, the composition comprises about 0.249 g of onapristone and about 0.784 g of pyrrolidone K29/32.
[0049] Further aspects provide methods of making amorphous onapristone by heating onapristone/pyrrolidone K29/32 until the pyrrolidone K29/32 melts forming a polymer melt, and the onapristone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone. In another aspect, the onapristone content of the glassy solid is about 24% w/w.
[0050] Another aspect provides compositions comprising onapristone, polyvinyl pyrrolidone K29/32, and polyethylene glycol 3350 (onapristone/pyrrolidone
K29/32/PEG). In another aspect, the composition comprises about 0.258 g of
onapristone, about 0.202 g of polyvinyl pyrrolidone K29/32, and about 0.503 g of polyethylene glycol 3350. In yet another aspect, the composition comprises about 0.242 g of onapristone, about 0.373 g of polyvinyl pyrrolidone K29/32, and about 0.384 g of polyethylene glycol 3350. In yet another aspect, the composition comprises about 0.241 g of onapristone, about 0.547 g of polyvinyl pyrrolidone K29/32, and about 0.197 g of polyethylene glycol 3350.
[0051] Further aspects provide methods of making amorphous onapristone by heating onapristone/pyrrolidone K29/32 until the polyvinyl pyrrolidone K29/32 and polyethylene glycol 3350 melts forming a polymer melt, and the onapristone dissolves in the polymer melt forming a mixture. Next, the mixture is allowed to cool to room temperature and form a glassy solid of amorphous onapristone.
[0052] Figure 1 shows X-ray powder diffraction patterns of onapristone as initially produced by the pH-cycle method, and stored under ambient conditions for 25 weeks, 43 weeks, and 16.5 months.
[0053] Figure 2 shows X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing polyvinyl pyrrolidone VA64) produced by the spray-drying method, and stored under ambient conditions for 12 weeks, 20 weeks, 36 weeks, and 15 months.
[0054] Figure 3 shows X-ray powder diffraction patterns of 25% w/w onapristone dispersions (containing hydroxypropyl methylcellulose succinate M) produced by the spray- drying method, and stored under ambient conditions for 12 weeks, 20 weeks, 36 weeks, and 15 months.
[0055] Figure 4 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing Kollidon® 30) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
[0056] Figure 5 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing polyvinyl pyrrolidone K29/32) produced by the hot- melt method, and stored under ambient conditions for 8 weeks and 8.5 months.
[0057] Figure 6 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing polyethylene glycol 8000) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months. The XRPD pattern for polyethylene glycol 8000 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
[0058] Figure 7 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months. The XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
[0059] Figure 8 shows X-ray powder diffraction patterns of nominal 25% w/w onapristone dispersions (containing 27.1% w/w polyvinyl pyrrolidone K29/32 and 72.9% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months. The XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
[0060] Figure 9 shows X-ray powder diffraction patterns of nominal 25%) w/w onapristone dispersions (containing 49.3% w/w polyvinyl pyrrolidone K29/32 and 50.7% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months. The XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
[0061] Figure 10 shows X-ray powder diffraction patterns of nominal 25%) w/w onapristone dispersions (containing 73.5% w/w polyvinyl pyrrolidone K29/32 and 26.5% w/w polyethylene glycol 3350) produced by the hot-melt method, and stored under ambient conditions for 8 weeks and 8.5 months. The XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes, demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient.
[0062] Figure 11 shows X-ray powder diffraction patterns of onapristone dispersions containing Kollidon® 30 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for Kollidon® 30 itself is shown for comparison purposes. [0063] Figure 12 shows X-ray powder diffraction patterns of onapristone dispersions containing polyvinylpyrrolidone K29/32 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for polyvinylpyrrolidone K29/32 itself is shown for comparison purposes.
[0064] Figure 13 shows X-ray powder diffraction patterns of onapristone dispersions containing polyethylene glycol 3350 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for polyethylene glycol 3350 itself is shown for comparison purposes (demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient).
[0065] Figure 14 shows X-ray powder diffraction patterns of onapristone dispersions containing polyethylene glycol 8000 produced by the solution-phase coprecipitate method. The nominal onapristone concentrations in the dispersions are indicated, and the XRPD pattern for polyethylene glycol 8000 itself is shown for comparison purposes (demonstrating that all scattering peaks in the XRPD of the formulations were due entirely to the excipient).
[0066] Figure 15 shows X-ray powder diffraction patterns of nominal 25% onapristone dispersions containing various amounts of Kollidon® 30 and polyethylene glycol 8000 produced by the solution-phase coprecipitate method. The relative percentages of the two polymers are indicated.
[0067] The onapristone amorphous forms can be used to treat a patient in need of treatment as described herein. The terms "treat," "prevent," or similar terms, as used herein, do not necessarily mean 100% or complete treatment or prevention. Rather, these terms refer to various degrees of treatment or prevention of a particular disease (e.g., 100%, 90%, 80%, 70%, 60%, 50%, 40%, 30%, 20%, 10%, 5%, or 1%) as recognized in the art as being beneficial. The terms "treatment" or "prevention" also refer to delaying onset of a disease for a period of time or delaying onset indefinitely. The term
"treatment" or "treating" refers to administering a drug or treatment to a patient or prescribing a drug to a patient where the patient or a third party (e.g., caretaker, family member, or health care professional) administers the drug or treatment. [0068] The onapristone amorphous forms also encompass derivatives. In one embodiment, the term "derivative" includes, but is not limited to, ether derivatives, acid derivatives, amide derivatives, ester derivatives and the like. Methods of preparing these derivatives are known to a person skilled in the art. For example, ether derivatives are prepared by the coupling of the corresponding alcohols. Amide and ester derivatives are prepared from the corresponding carboxylic acid by a reaction with amines and alcohols, respectively.
[0069] The onapristone amorphous forms also encompass hydrates or solvates of onapristone amorphous or crystalline forms (e.g., hemihydrate, monohydrate, dihydrate, trihydrate and the like). Hydrates or solvates of onapristone may be prepared by contacting onapristone with water or a solvent under suitable conditions to produce the hydrate or solvate of choice, for example, as described herein.
[0070] The onapristone amorphous forms also encompass metabolites of onapristone amorphous forms. "Metabolite" or "metabolites" refer to any substance produced from another substance by metabolism or a through a metabolic process of a living cell or organ.
[0071] Any of the amorphous onapristone forms described herein can be
administered or used as starting materials to be administered orally, parenterally (IV, IM, depot-DVI, SQ, and depot-SQ), sublingually, intranasally (inhalation), intrathecally, topically, or rectally. Dosage forms known to those of skill in the art are suitable for delivery of the onapristone amorphous forms described herein.
[0072] The onapristone amorphous compounds can be formulated into suitable pharmaceutical preparations such as tablets, capsules, or elixirs for oral administration or in sterile solutions or suspensions for parenteral administration. The onapristone amorphous compounds described herein can be formulated into pharmaceutical compositions using techniques and procedures well known in the art.
[0073] In one aspect, about 10 to about 200 mg of the onapristone amorphous compounds, or a physiologically acceptable salt, pro-drug, or co-crystal thereof can be compounded or used as a starting material for compounding with a physiologically acceptable vehicle, carrier, excipient, binder, preservative, stabilizer, flavor, etc., in a unit dosage form as called for by accepted pharmaceutical practice. The amount of active substance in compositions or preparations comprising the onapristone amorphous compounds is such that a suitable dosage in the range indicated is obtained.
[0074] In another aspect, the compositions can be formulated in a unit dosage form, each dosage containing from about 1 mg to about 1.2 g, or about 2.5 to about 200 mg of the active ingredient. The term "unit dosage from" refers to physically discrete units suitable as unitary dosages for human subjects and other mammals, each unit containing a predetermined quantity of active material calculated to produce the desired therapeutic effect, in association with one or more suitable pharmaceutical excipients.
[0075] In one aspect, one or more of the onapristone amorphous compounds are mixed with or used as starting materials mixed with a suitable pharmaceutically acceptable carrier to form compositions. Upon mixing or addition of the compound(s), the resulting mixture may be a solution, suspension, emulsion, or the like. Liposomal suspensions may also be used as pharmaceutically acceptable carriers. These may be prepared according to methods known to those skilled in the art. The form of the resulting mixture depends upon a number of factors, including the intended mode of administration and the solubility of the compound in the selected carrier or vehicle. In one aspect, the effective concentration is sufficient for lessening or ameliorating at least one symptom of the disease, disorder, or condition treated and may be empirically determined.
[0076] Pharmaceutical carriers or vehicles suitable for administration of the onapristone amorphous compounds described herein include any such carriers suitable for the particular mode of administration. In addition, the active materials can also be mixed with other active materials that do not impair the desired action, or with materials that supplement the desired action, or have another action. The compounds may be formulated as the sole pharmaceutically active ingredient in the composition or may be combined with other active ingredients.
[0077] In another aspect, if the onapristone amorphous compounds exhibit insufficient solubility, methods for solubilizing may be used. Such methods are known and include, but are not limited to, using co-solvents such as dimethylsulfoxide (DMSO), using surfactants such as TWEEN, and dissolution in aqueous sodium bicarbonate. Derivatives of the compounds, such as salts or prodrugs, may also be used in formulating effective pharmaceutical compositions.
[0078] The concentration of the compound is effective for delivery of an amount upon administration that lessens or ameliorates at least one symptom of the disorder for which the compound is administered. Typically, the compositions are formulated for single dosage administration.
[0079] In another aspect, the onapristone amorphous compounds described herein may be prepared with carriers that protect them against rapid elimination from the body, such as time-release formulations or coatings. Such carriers include controlled release formulations, such as, but not limited to, microencapsulated delivery systems. The active compound can be included in the pharmaceutically acceptable carrier in an amount sufficient to exert a therapeutically useful effect in the absence of undesirable side effects on the patient treated. The therapeutically effective concentration may be determined empirically by testing the compounds in known in vitro and in vivo model systems for the treated disorder.
[0080] In another aspect, the onapristone amorphous compounds and compositions described herein can be enclosed in multiple or single dose containers. The enclosed compounds and compositions can be provided in kits, for example, including component parts that can be assembled for use. For example, an onapristone amorphous compound can be used as a starting material for a lyophilized form and a suitable diluent may be provided as a separated component for combination prior to use. A kit may include onapristone amorphous compound and a second therapeutic agent for co-administration. The onapristone amorphous compound and second therapeutic agent may be provided as separate component parts. A kit may include a plurality of containers, each container holding one or more unit dose of the onapristone amorphous compounds described herein. In one aspect, the containers can be adapted for the desired mode of
administration, including, but not limited to tablets, gel capsules, sustained-release capsules, and the like for oral administration; depot products, pre-filled syringes, ampoules, vials, and the like for parenteral administration; and patches, medipads, creams, and the like for topical administration. [0081] The concentration of the onapristone amorphous compound in the
pharmaceutical composition will depend on dissolution, absorption, metabolism, and excretion rates of the active compound, the dosage schedule, and amount administered as well as other factors known to those of skill in the art.
[0082] In another aspect, the active ingredient may be administered at once, or may be divided into a number of smaller doses to be administered at intervals of time. It is understood that the precise dosage and duration of treatment is a function of the disease being treated and may be determined empirically using known testing protocols or by extrapolation from in vivo or in vitro test data. It is to be noted that concentrations and dosage values may also vary with the severity of the condition to be alleviated. It is to be further understood that for any particular subject, specific dosage regimens should be adjusted over time according to the individual need and the professional judgment of the person administering or supervising the administration of the compositions, and that the concentration ranges set forth herein are exemplary only and are not intended to limit the scope or practice of the claimed compositions.
[0083] If oral administration is desired, the compound can be provided in a composition that protects it from the acidic environment of the stomach. For example, the composition can be formulated in an enteric coating that maintains its integrity in the stomach and releases the active compound in the intestine. The composition may also be formulated in combination with an antacid or other such ingredient.
[0084] Oral compositions will generally include an inert diluent or an edible carrier and may be compressed into tablets or enclosed in gelatin capsules. For the purpose of oral therapeutic administration, the active compound or compounds can be incorporated with excipients and used in the form of tablets, capsules, or troches. Pharmaceutically compatible binding agents and adjuvant materials can be included as part of the composition.
[0085] The tablets, pills, capsules, troches, and the like can contain any of the following ingredients or compounds of a similar nature: a binder such as, but not limited to, gum tragacanth, acacia, corn starch, or gelatin; an excipient such as microcrystalline cellulose, starch, or lactose; a disintegrating agent such as, but not limited to, alginic acid and corn starch; a lubricant such as, but not limited to, magnesium stearate; a glidant, such as, but not limited to, colloidal silicon dioxide; a sweetening agent such as sucrose or saccharin; and a flavoring agent such as peppermint, methyl salicylate, or fruit flavoring.
[0086] When the dosage unit form is a capsule, it can contain, in addition to material of the above type, a liquid carrier such as a fatty oil. In addition, dosage unit forms can contain various other materials, which modify the physical form of the dosage unit, for example, coatings of sugar and other enteric agents. The compounds can also be administered as a component of an elixir, suspension, syrup, wafer, chewing gum or the like. A syrup may contain, in addition to the active compounds, sucrose as a sweetening agent and certain preservatives, dyes and colorings, and flavors.
[0087] The active materials can also be mixed with other active materials that do not impair the desired action, or with materials that supplement the desired action. The onapristone amorphous compounds can be used, for example, in combination with an antitumor agent, a hormone, a steroid, or a retinoid. The antitumor agent may be one of numerous chemotherapy agents (e.g., everolimus, trastuzumab, TM1-D, anti-HER2 drugs, bevacizumab, paclitaxel, docetaxel, taxanes, doxorubicin, liposomal doxorubicin, pegylated liposomal doxorubicin, anthracyclines, anthracenediones, carboplatin, cisplatin, 5-FU, gemcitabine and cyclophosphamide).
[0088] In one aspect, solutions or suspensions used for parenteral, intradermal, subcutaneous, or topical application can include any of the following components: a sterile diluent such as water for injection, saline solution, fixed oil, a naturally occurring vegetable oil such as sesame oil, coconut oil, peanut oil, cottonseed oil, and the like, or a synthetic fatty vehicle such as ethyl oleate, and the like, polyethylene glycol, glycerin, propylene glycol, or other synthetic solvent; antimicrobial agents such as benzyl alcohol and methyl parabens; antioxidants such as ascorbic acid and sodium bisulfite; chelating agents such as ethylenediaminetetraacetic acid (EDTA) or its disodium salt; buffers such as acetates, citrates, and phosphates; and agents for the adjustment of tonicity such as sodium chloride and dextrose. Parenteral preparations can be enclosed in ampoules, disposable syringes, or multiple dose vials made of glass, plastic, or other suitable material. Buffers, preservatives, antioxidants, and the like can be incorporated as required.
[0089] Where administered intravenously, suitable carriers include, but are not limited to, physiological saline, phosphate buffered saline (PBS), and solutions containing thickening and solubilizing agents such as glucose, polyethylene glycol, polypropylene glycol, and mixtures thereof. Liposomal suspensions including tissue- targeted liposomes may also be suitable as pharmaceutically acceptable carriers. These may be prepared according to methods known in the art.
[0090] In another aspect, the onapristone amorphous compounds may be prepared with carriers that protect the compound against rapid elimination from the body, such as time-release formulations or coatings. Such carriers include controlled release formulations, such as, but not limited to, implants and microencapsulated delivery systems, and biodegradable, biocompatible polymers such as collagen, ethylene vinyl acetate, polyanhydrides, polyglycolic acid, polyorthoesters, polylactic acid, hydroxyl propyl methyl cellulose (HPMC), other cellulose derivatives, and the like. Methods for preparation of such formulations are known to those skilled in the art.
[0091] In yet another aspect, compounds employed in the methods of the disclosure may be administered enterally or parenterally. When administered orally, compounds employed in the methods of the disclosure can be administered in usual dosage forms for oral administration as is well known to those skilled in the art. These dosage forms include the usual solid unit dosage forms of tablets and capsules as well as liquid dosage forms such as solutions, suspensions, and elixirs. When the solid dosage forms are used, they can be of the sustained release type so that the compounds employed in the methods described herein need to be administered only once or twice daily.
[0092] The oral dosage forms can be administered to the patient 1, 2, 3, or 4 times daily. The onapristone amorphous compounds described herein can be administered either three or fewer times, or even once or twice daily. Hence, the onapristone employed in the methods of the disclosure be administered in oral dosage form. Whatever oral dosage form is used, they can be designed so as to protect the compounds employed in the methods described herein from the acidic environment of the stomach. Enteric coated tablets are well known to those skilled in the art. In addition, capsules filled with small spheres each coated to protect from the acidic stomach, are also well known to those skilled in the art.
[0093] The terms "therapeutically effective amount" and "therapeutically effective period of time" are used to denote treatments at dosages and for periods of time effective to reduce neoplastic cell growth. As noted above, such administration can be parenteral, oral, sublingual, transdermal, topical, intranasal, or intrarectal. In one aspect, when administered systemically, the therapeutic composition can be administered at a sufficient dosage to attain a blood level of the compounds of from about 0.01 μΜ to about 20 μΜ. For localized administration, much lower concentrations than this can be effective, and much higher concentrations may be tolerated. One of skill in the art will appreciate that such therapeutic effect resulting in a lower effective concentration of the ONA
amorphous compound may vary considerably depending on the tissue, organ, or the particular animal or patient to be treated. It is also understood that while a patient may be started at one dose, that dose may be varied overtime as the patient's condition changes. In one aspect, the onapri stone amorphous compounds can be used to inhibit the growth of tumors derived from tissue including, but not limited to, breast, brain, meningiomas, prostate, ovarian, endometrial, uterine leiomyoma, lung, and uterine tissues.
[0094] It should be apparent to one skilled in the art that the exact dosage and frequency of administration will depend on the particular compounds employed in the methods of the disclosure administered, the particular condition being treated, the severity of the condition being treated, the age, weight, general physical condition of the particular patient, and other medication the individual may be taking as is well known to administering physicians who are skilled in this art.
EXAMPLES
[0095] Example 1
[0096] Physical Form of Onapristone Compound
[0097] The physical form of onapristone, either as the bulk drug substance or in its compositions, was established using X-ray powder diffraction (XRPD). XRPD patterns were obtained using a Rigaku MiniFlex powder diffraction system, equipped with a horizontal goniometer operating in the Θ/2Θ mode. The X-ray source was nickel-filtered Ka emission of copper (1.54184 A). Samples were packed into the sample holder using a back-fill procedure, and were scanned over the range of 3.5 to 40 degrees 2Θ at a scan rate of 0.5 degrees 29/min. Using a data acquisition rate of 1 point per second, these scanning parameters equate to a step size of 0.0084 degrees 2Θ. Calibration of the diffractometer system was effected using purified talc as a reference material. The intensity scale for all diffraction patterns was normalized so that the relative intensity of the most intense peak in the pattern equaled 100%.
[0098] Example 2
[0099] The pH-Cycle Method to Obtain Amorphous Onapri stone
[00100] The onapristone molecule contains a functional group that is effectively a substituted aniline:
Figure imgf000020_0001
[00101] In one aspect, one would expect this group to be somewhat acidic. Using the pKa-Predictor module of the Physical Chemistry Program Suite (Advanced Chemical Laboratories, Toronto, CA), the pKa of this group was predicted to be 5.30 ± 0.25. Using the predictive solubility module of the ACD program, it was determined that the protonated form of the compound is expected to be fairly soluble in water, while the neutral form is expected to be relatively insoluble in water.
[00102] In one aspect, 0.408 g of onapristone (0.91 mmol) was slurried in 25 mL of water, and then 0.5 mL of 2N HC1 (1.0 mmol) was added. The solid completely dissolved in approximately 5 minutes, whereupon 2.0 mL of 0.5 N NaOH (1.0 mmol) was added. The precipitated onapristone was suction-filtered, and allowed to air-dry overnight.
[00103] The XRPD pattern of this product was obtained, and the lack of sharp scattering peaks demonstrated its amorphous character. After the initial characterization, the substance was placed in a glass vial, and stored under ambient conditions
(temperature of 22-24°C). The product was subsequently obtained after storage under ambient conditions for 25 weeks, 43 weeks, and 16.5 months. As shown in Figure 1, the pH-cycled onapnstone remained amorphous over the entire 16.5 month storage period.
[00104] Example 3
[00105] Spray-Drying Method to Obtain Amorphous Onapristone
[00106] Two samples of onapristone that had been spray-dried with excipients were prepared to have the following compositions:
[00107] Sample ID = SSF-PDS-027-001A comprising 25% onapristone in a matrix consisting of PVP VA64, and was spray-dried from a solution consisting of 8% w/w solids in methanol.
[00108] Sample ID = SSF-PDS-027-001B comprising 25% onapristone in a matrix consisting of HPMCAS-M, and was spray-dried from a solution consisting of 8% w/w solids in methanol.
[00109] XRPD patterns of these samples were obtained when initially received and after 12 weeks, 20 weeks, 36 weeks, and 15 months had elapsed. The XRPD patterns obtained for sample SSF-PDS-027-001A are collected in Figure 2, while the XRPD patterns obtained for sample SSF-PDS-027-001B are collected in Figure 3.
[00110] Examination of Figures 2 and 3 reveals that both spray-dried dispersions were amorphous when initially prepared, and that they both remained amorphous over the 315 month storage period.
[00111] Example 4
[00112] Hot-Melt Method to Obtain Amorphous Onapristone [00113] Binary Formulations
[00114] Four formulations were prepared to determine if a hot-melt procedure was capable of producing dispersions containing amorphous onapristone. The experimental details associated with these formulations are as follows: [00115] Preparation 1 : 0.255 g of onapristone and 0.777 g of Kollidon® 30 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymer had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 24.7% w/w.
[00116] Preparation 2: 0.241 g of onapristone and 0.700 g of polyethylene glycol 8000 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymer had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 25.6% w/w.
[00117] Preparation 3: 0.238 g of onapristone and 0.762 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymer had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 23.8% w/w.
[00118] Preparation 4: 0.249 g of onapristone and 0.784 g of polyvinyl pyrrolidone K29/32 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymer had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 24.1% w/w.
[00119] The XRPD pattern of formulations containing polyvinyl pyrrolidone (i.e., preparations 1 and 4) are shown in Figures 4 and 5, respectively. Also shown in Figures 4 and 5 are the XRPD patterns of the same products after each had been stored under ambient conditions for time periods of 8 weeks and 8.5 months. Since no sharp peaks attributable to crystalline onapristone were detected in the XRPD of the preparations, it is concluded that the drug substance remained amorphous over the entire 8.5 month storage period.
[00120] The XRPD pattern of formulations containing polyethylene glycol (i.e., preparations 2 and 3) are shown in Figures 6 and 7. Also shown in Figures 6 and 7 are the XRPD patterns of the same products after each had been stored under ambient conditions for time periods of 8-weeks and 8.5 months, as well as the XRPD patterns of the polyethylene glycol polymers used to form the products.
[00121] In addition to a number of weak scattering features, the XRPD patterns of the PEG polymer products are dominated by two scattering peaks at approximately 19 and 23 degrees 2Θ. All of the polymer peaks were observed in the XRPD patterns of the dispersions, but no additional peaks attributable to crystalline onapristone were detected in the XRPD patterns of the preparations. Therefore, the drug substance remained amorphous over the entire 8.5 month storage period.
[00122] Ternary Formulations
[00123] Three additional formulations were prepared to determine if the inclusion of varying amounts of polyethylene glycol could produce less brittle dispersions for products prepared using the hot-melt procedure. The experimental details associated with these formulations are as follows:
[00124] Preparation 5: 0.258 g of onapristone, 0.202 g of polyvinyl pyrrolidone K29/32, and 0.543 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymers had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 25.7% w/w, and the PVP content in this sample was 27.1% w/w (relative to the total polymer concentration).
[00125] Preparation 6: 0.242 g of onapristone, 0.373 g of polyvinyl pyrrolidone K29/32, and 0.384 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymers had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 24.2% w/w, and the PVP content in this sample was 49.3% w/w (relative to the total polymer concentration).
[00126] Preparation 7: 0.241 g of onapristone, 0.547 g of polyvinyl pyrrolidone K29/32, and 0.197 g of polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and then heated on a hot plate until the polymers had melted and the onapristone dissolved in the melt. After that, the beaker and contents were allowed to cool back to room temperature, whereupon the glassy solid was broken up and then ground into a powder. The onapristone content of this sample was 24.5% w/w, and the PVP content in this sample was 73.5% w/w (relative to the total polymer concentration).
[00127] The XRPD patterns of these latter three preparations are shown in Figures 8-10, respectively, along with the XRPD patterns of the polyethylene glycol 3350 excipient. Also shown in Figures 8-10 are the XRPD patterns of the same products after each had been stored under ambient conditions for time periods of 8 weeks and 8.5 months. The XRPD patterns of the hot-melt dispersions were dominated by the two scattering peaks (at approximately 19 and 23 degrees 2Θ) associated with the PEG-3350, but no additional peaks attributable to crystalline onapristone were detected in the XRPD of the preparations. Therefore, the drug substance remained amorphous over the 8 week storage period. In addition, all three dispersions were easily dislodged from the beaker, and their rendition into powder was straight-forward.
[00128] Example 5
[00129] Solution-Phase Method to Obtain Amorphous Onapristone [00130] Binary Formulations
[00131] Four formulation systems were prepared to determine if a solution-phase procedure was capable of producing dispersions containing amorphous onapristone. Each system was based on the use of a specific polymer, but containing different amounts of onapristone. The experimental details associated with these formulations are as follows.
[00132] For preparations within the Kollidon® 30 system, the requisite amount of onapristone and Kollidon® 30 were weighed directly into a 150 mL beaker, and 30 mL of absolute isopropanol was added to the beaker. The contents were stirred until dissolution was complete, whereupon the solution was poured into an evaporating dish and allowed to completely air-dry. The Kollidon® 30 preparations had the following compositions:
Figure imgf000025_0001
The XRPD patterns obtained for the Kollidon® 30 formulation series are shown in Figure 11. Since no sharp peaks attributable to crystalline onapristone were detected in the XRPD of the preparations, it was concluded that the drug substance was amorphous in the products.
[00133] For preparations within the polyvinylpyrrolidone K29/32 system, the requisite amount of onapristone and Kollidon® 30 were weighed directly into a 150 mL beaker, and 30 mL of absolute isopropanol was added to the beaker. The contents stirred until dissolution was complete, whereupon the solution was poured into an evaporating dish and allowed to completely air-dry. The polyvinylpyrrolidone K29/32 preparations had the following compositions:
Nominal Mass Mass PVP Actual Polymer Onapri stone K29/32 Polymer Percentage Taken (g) Taken (g) Percentage
6 0.0313 0.4717 6.22
12 0.0604 0.4399 12.07
18 0.0903 0.4087 18.10
24 0.1212 0.3881 23.80
The XRPD patterns obtained for the polyvinylpyrrolidone K29/32 formulation series are shown in Figure 12. Since no sharp peaks attributable to crystalline onapristone were detected in the XRPD of the preparations, it was concluded that the drug substance was amorphous in the products.
[00134] For preparations within the polyethylene glycol 3350 system, the requisite amount of onapristone and polyethylene glycol 3350 were weighed directly into a 150 mL beaker, and 30 mL of absolute isopropanol was added to the beaker. The contents were heated and stirred until dissolution was complete, whereupon the solution was poured into an evaporating dish and allowed to completely air-dry. The polyethylene glycol 3350 preparations had the following compositions:
Figure imgf000026_0001
The XRPD patterns obtained for the polyethylene glycol 3350 formulation series are shown in Figure 13. All of the observed scattering peaks were associated with the polyethylene glycol 3350, and no sharp peaks attributable to crystalline onapristone were detected in the XRPD of the preparations. The drug substance was amorphous in the products.
[00135] For preparations within the polyethylene glycol 8000 system, the requisite amount of onapristone and polyethylene glycol 8000 were weighed directly into a 150 mL beaker, and 30 mL of absolute isopropanol was added to the beaker. The contents were heated and stirred until dissolution was complete, whereupon the solution was poured into an evaporating dish and allowed to completely air-dry. The polyethylene glycol 8000 preparations had the following compositions:
Figure imgf000027_0001
The XRPD patterns obtained for the polyethylene glycol 8000 formulation series are shown in Figure 14. All of the observed scattering peaks were associated with the polyethylene glycol 8000, and no sharp peaks attributable to crystalline onapristone were detected in the XRPD of the preparations. The drug substance was amorphous in the products.
[00136] Ternary Formulations
[00137] Since coprecipitate formulations with superior handling characteristics can often be prepared through the use of more than one polymer, the Kollidon® 30 / polyethylene glycol 8000 system was studied to determine if a solution-phase procedure was capable of producing dispersions containing amorphous onapristone. The systems contained a nominal 25% amount of onapristone, and had the following compositions: Mass
Nominal Mass Actual Mass PEG Actual
Kollidon®
PVP/PEG Onapristone Onapristone 8000 Polymer
30 Taken
Percentage Taken (g) Percentage Taken (g) Percentages
(g)
26% PVP / PVP=26.14%
0.128 24.52 0.103 0.291 74% PEG PEG=73.86%
50% PVP / PVP=49.75%
0.123 23.61 0.198 0.200 50% PEG PEG=50.25%
74% PVP / PVP=74.11%
0.123 22.61 0.312 0.109 26% PEG PEG=25.89%
The XRPD patterns obtained for the solution-phase ternary coprecipitate formulations are shown in Figure 15. All of the observed scattering peaks were associated with the polyethylene glycol 8000, and no sharp peaks attributable to crystalline onapristone were detected in the XRPD of the preparations. The drug substance was amorphous in the ternary products.
[00138] Although the above description refers to particular aspects, it is to be understood that these aspects are merely illustrative. It will be apparent to those skilled in the art that various modifications and variations can be made to the amorphous forms and methods described herein. Thus, it is intended that the present description include modifications and variations that are within the scope of the appended claims and their equivalents.

Claims

CLAIMS What is claimed is:
1. A method of making amorphous onapri stone comprising: dissolving onapristone in water to form an onapristone solution; adding an acid to the onapristone solution wherein the pH is reduced; adding a base to the onapristone solution wherein the pH is increased; and precipitating onapristone from the solution to form amorphous onapristone, wherein the XPRD pattern of the precipitated onapristone does not produce any substantially sharp scatter peaks.
2. The method of claim 1, wherein the acid solution comprises an acid selected from the group consisting of hydrochloric acid, nitric acid, and sulfuric acid.
3. The method of claim 1, wherein the base is selected from the group consisting of sodium hydroxide, potassium hydroxide, and ammonium hydroxide.
4. The method of claim 1 wherein the pH is reduced to 1 or below and the pH is increased to 10 or above.
5. A method of making amorphous onapristone comprising: dissolving onapristone in a solvent selected from the group consisting of acetonitrile, ethanol, acetone, or isopropanol to form an onapristone solution; and drying the onapristone solution to form amorphous onapristone wherein no detectable crystalline solvates are formed.
6. A composition comprising onapristone (25%) in a PVP VA64 copolymer matrix.
7. A method of spray drying amorphous onapristone comprising, spray drying the composition of claim 6 from a solution comprising about 8% w/w solids in methanol wherein the onapristone is amorphous.
8. A composition comprising onapristone and polyvinylpyrrolidone.
9. The composition of claim 8, further comprising about 0.255 g of onapristone and about 0.777 g of polyvinylpyrrolidone.
10. A method of making amorphous onapristone comprising: heating the composition of claim 8 until the polyvinylpyrrolidone 30 melts and forms a polymer melt and the onapristone dissolves in the polymer melt forming a mixture; and allowing the mixture to cool to room temperature and form a glassy solid comprising amorphous onapristone.
11. The method of claim 10, wherein the onapristone content of the glassy solid is about 24% w/w.
12. A composition comprising onapristone and polyethylene glycol 8000.
13. The composition of claim 12, further comprising about 0.241 g of onapristone and about 0.700 g of polyethylene glycol 8000.
14. A method of making amorphous onapristone comprising: heating the composition of claim 12 until the polyethylene glycol 8000 melts and forms a polymer melt and the onapristone dissolves in the polymer melt forming a mixture; and allowing the mixture to cool to room temperature and form a glassy solid comprising amorphous onapristone.
15. The method of claim 14, wherein the onapristone content of the glassy solid is about 25% w/w.
16. A composition comprising onapristone and polyethylene glycol 3350.
17. The composition of claim 16, further comprising about 0.238 g of onapristone and about 0.762 g of polyethylene glycol 3350.
18. A method of making amorphous onapristone comprising: heating the composition of claim 16 until the polyethylene glycol 3350 melts and forms a polymer melt and the onapristone dissolves in the polymer melt forming a mixture; and allowing the mixture to cool to room temperature and form a glassy solid comprising amorphous onapristone.
19. The method of claim 18, wherein the onapristone content of the glassy solid is about 23% w/w.
20. A composition comprising onapristone and pyrrolidone K29/32.
21. The composition of claim 20, further comprising about 0.249 g of onapristone and about 0.784 g of pyrrolidone K29/32.
22. A method of making amorphous onapristone comprising: heating the composition of claim 20 until the pyrrolidone K29/32 melts and forms a polymer melt and the onapristone dissolves in the polymer melt forming a mixture; and allowing the mixture to cool to room temperature and form a glassy solid comprising amorphous onapristone.
23. The method of claim 22, wherein the onapristone content of the glassy solid is about 24% w/w.
24. A composition comprising onapristone, polyvinyl pyrrolidone K29/32, and polyethylene glycol 3350.
25. The composition of claim 24, further comprising about 0.258 g of onapristone, about 0.202 g of polyvinyl pyrrolidone K29/32, and about 0.503 g of polyethylene glycol 3350.
26. The composition of claim 24, further comprising about 0.242 g of onapristone, about 0.373 g of polyvinyl pyrrolidone K29/32, and about 0.384 g of polyethylene glycol 3350.
27. The composition of claim 24, further comprising about 0.241 g of onapristone, about 0.547 g of polyvinyl pyrrolidone K29/32, and about 0.197 g of polyethylene glycol 3350.
28. A method of making amorphous onapristone comprising: heating the composition of claim 24 until the polyvinyl pyrrolidone K29/32 and polyethylene glycol 3350 melts and forms a polymer melt, and the onapristone dissolves in the polymer melt forming a mixture; and allowing the mixture to cool to room temperature and form a glassy solid comprising amorphous onapristone.
PCT/US2016/066420 2015-12-15 2016-12-13 Amorphous onapristone compositions and methods of making the same WO2017106214A1 (en)

Priority Applications (9)

Application Number Priority Date Filing Date Title
MX2018007154A MX2018007154A (en) 2015-12-15 2016-12-13 Amorphous onapristone compositions and methods of making the same.
CA3008422A CA3008422A1 (en) 2015-12-15 2016-12-13 Amorphous onapristone compositions and methods of making the same
AU2016370499A AU2016370499B2 (en) 2015-12-15 2016-12-13 Amorphous onapristone compositions and methods of making the same
EP16876503.0A EP3389632A4 (en) 2015-12-15 2016-12-13 Amorphous onapristone compositions and methods of making the same
CN201680077010.2A CN108883067B (en) 2015-12-15 2016-12-13 Amorphous onapristone composition and preparation method thereof
JP2018532190A JP2019503353A (en) 2015-12-15 2016-12-13 Amorphous onapristone composition and method of making the same
KR1020187019175A KR20180113988A (en) 2015-12-15 2016-12-13 Amorphous Ona Pristone Composition and Method of Manufacturing the Same
HK18114258.8A HK1255104A1 (en) 2015-12-15 2018-11-08 Amorphous onapristone compositions and methods of making the same
HK18115767.9A HK1256633A1 (en) 2015-12-15 2018-12-10 Amorphous onapristone compositions and methods of making the same

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
US201562267540P 2015-12-15 2015-12-15
US62/267,540 2015-12-15

Publications (1)

Publication Number Publication Date
WO2017106214A1 true WO2017106214A1 (en) 2017-06-22

Family

ID=59057809

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/US2016/066420 WO2017106214A1 (en) 2015-12-15 2016-12-13 Amorphous onapristone compositions and methods of making the same

Country Status (10)

Country Link
US (2) US10548905B2 (en)
EP (1) EP3389632A4 (en)
JP (1) JP2019503353A (en)
KR (1) KR20180113988A (en)
CN (1) CN108883067B (en)
AU (1) AU2016370499B2 (en)
CA (1) CA3008422A1 (en)
HK (2) HK1255104A1 (en)
MX (1) MX2018007154A (en)
WO (1) WO2017106214A1 (en)

Families Citing this family (5)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US10786461B2 (en) 2014-11-17 2020-09-29 Context Biopharma Inc. Onapristone extended-release compositions and methods
BR112018005999A2 (en) 2015-09-25 2019-01-08 Context Biopharma Inc methods for the production of onapristone intermediates
KR20180113988A (en) 2015-12-15 2018-10-17 컨텍스트 바이오파마 인코포레이티드 Amorphous Ona Pristone Composition and Method of Manufacturing the Same
US20180148471A1 (en) 2016-11-30 2018-05-31 Arno Therapeutics, Inc. Methods for onapristone synthesis dehydration and deprotection
WO2023172909A1 (en) * 2022-03-08 2023-09-14 Context Biopharma Inc. Compositions comprising anti-progestins and selective estrogen receptor modulators and methods of using the same

Citations (11)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5141961A (en) * 1991-06-27 1992-08-25 Richrdson-Vicks Inc. Process for solubilizing difficulty soluble pharmaceutical actives
EP0803250A1 (en) * 1996-04-24 1997-10-29 American Home Food Products, Inc. Controlled release of steroids from sugar coatings
US6143754A (en) * 1994-10-24 2000-11-07 Schering Aktiengesellschaft Competitive progesterone antagonist for demand-oriented female birth control
US6537584B1 (en) * 1999-11-12 2003-03-25 Macromed, Inc. Polymer blends that swell in an acidic environment and deswell in a basic environment
WO2006010097A2 (en) * 2004-07-09 2006-01-26 The Population Council, Inc. Sustained release compositions containing progesterone receptor modulators
WO2006111856A1 (en) * 2005-04-20 2006-10-26 Pfizer Limited Pyrazole derivatives as progesterone receptor antagonists
US20070166372A1 (en) * 2006-01-19 2007-07-19 Mai De Ltd. Preparation of solid coprecipitates of amorphous valsartan
US20120140790A1 (en) * 2009-12-15 2012-06-07 Ali Mir M Therapeutic Polymeric Nanoparticle Compositions with High Glass Transition Termperature or High Molecular Weight Copolymers
WO2012083017A2 (en) * 2010-12-16 2012-06-21 Celgene Corporation Controlled release oral dosage forms of poorly soluble drugs and uses thereof
WO2014093918A1 (en) * 2012-12-13 2014-06-19 Warsaw Orthopedic, Inc. Compositions and methods comprising polyethylene glycol and magnesium for treatment of neuronal injury
US9193757B2 (en) * 2013-03-12 2015-11-24 Arno Therapeutics, Inc. Onapristone polymorphic forms and methods of use

Family Cites Families (59)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE3321826A1 (en) 1983-06-15 1984-12-20 Schering AG, 1000 Berlin und 4709 Bergkamen 13 alpha -Alkylgonanes, the preparation thereof and pharmaceutical products containing these
US4780461A (en) 1983-06-15 1988-10-25 Schering Aktiengesellschaft 13α-alkyl-gonanes, their production, and pharmaceutical preparations containing same
ES533260A0 (en) 1983-06-15 1985-02-01 Schering Ag PROCEDURE FOR THE PREPARATION OF 13A-ALQUILGONANOS
US4742000A (en) 1986-05-02 1988-05-03 University Of Chicago Antibody to human progesterone receptor and diagnostic materials and methods
DE3630030A1 (en) 1986-09-01 1988-03-03 Schering Ag 13 (ALPHA) -ALKYLGONAN- (DELTA) (UP ARROW) 9 (UP ARROW) (UP ARROW) ((UP ARROW) (UP ARROW) 1 (UP ARROW) 1 (UP ARROW)) (UP ARROW) -5, 10-EPOXIDE
US4774236A (en) 1986-09-17 1988-09-27 Research Triangle Institute 17α-(substituted-methyl)-17β-hydroxy/esterified hydroxy steroids and pharmaceutical compositions containing them
IE60780B1 (en) 1987-01-23 1994-08-10 Akzo Nv New 11-aryl steroid derivatives
DE3822770A1 (en) 1988-07-01 1990-01-04 Schering Ag 13-ALKYL-11SS-PHENYLGONANE
US5283190A (en) 1989-07-31 1994-02-01 Traish Adbulmaged M Specific monoclonal antibodies against a defined epitope of progesterone receptor and methods for their use
DE4008584A1 (en) 1990-03-15 1991-09-26 Schering Ag METHOD FOR PRODUCING INTERMEDIATE PRODUCTS FOR THE ANTIGESTAGE SYNTHESIS (ONAPRISTONE SYNTHESIS)
MX9301121A (en) 1992-03-02 1993-09-01 Schering Ag METHOD AND EQUIPMENT FOR ORAL CONTRACEPTION AND REGULATION OF MENSTRUATION WITH ESTROGEN / PROGESTIN / ANIPROGESTIN.
CN1053450C (en) 1992-11-19 2000-06-14 北京第三制药厂 Total synthesis method of 17-substituted 11 beta-substituted aromatic group-4, 9-estradiene compound
DE4332283A1 (en) 1993-09-20 1995-04-13 Jenapharm Gmbh Novel 11-benzaldoximestradiene derivatives, processes for their preparation and medicaments containing these compounds
US6900193B1 (en) 1996-05-01 2005-05-31 The United States Of America As Represented By The Department Of Health And Human Services Structural modification of 19-norprogesterone I: 17-α-substituted-11-β-substituted-4-aryl and 21-substituted 19-norpregnadienedione as new antiprogestational agents
IL122740A (en) 1997-01-15 2003-09-17 Akzo Nobel Nv 16-hydroxy-11-(substituted phenyl)-estra-9,4-diene derivatives, their preparation and pharmaceutical compositions containing them
US5962444A (en) 1998-05-29 1999-10-05 Research Triangle Institute 17β-nitro-11β-arylsteroids and their derivatives having agonist or antagonist hormonal properties
CA2407556C (en) 2000-05-19 2011-06-21 Genentech, Inc. Gene detection assay for improving the likelihood of an effective response to an erbb antagonist cancer therapy
US6750015B2 (en) 2000-06-28 2004-06-15 Kathryn B. Horwitz Progesterone receptor-regulated gene expression and methods related thereto
UY26966A1 (en) 2000-10-18 2002-06-20 Schering Ag USE OF ANTIPROGESTINES FOR THE INDUCTION OF APOPTOSIS IN A CELL
US7381976B2 (en) 2001-03-13 2008-06-03 Triton Thalassic Technologies, Inc. Monochromatic fluid treatment systems
US7105642B2 (en) 2001-08-03 2006-09-12 Cell Signalling Technology, Inc. Monoclonal antibodies specific for phosphorylated estrogen receptor alpha (Ser118) and uses thereof
US20040121304A1 (en) 2001-12-21 2004-06-24 Ulrike Fuhrmann Method for screening for progesterone receptor isoform-specific ligands and for tissue-selective progesterone receptor ligands
EP1613640A4 (en) 2003-02-28 2010-05-19 Us Gov Health & Human Serv Method for preparing 17 alpha-acetoxy-11 beta-(4-n,n-dimethylamin ophenyl)-19-norpregna-4,9-diene-3,20-dione, intermediates thereof, and methods for the preparation of such intermediates
US20040265371A1 (en) 2003-06-25 2004-12-30 Looney Dwayne Lee Hemostatic devices and methods of making same
CA2580795A1 (en) 2004-09-22 2006-04-06 Tripath Imaging, Inc. Methods and compositions for evaluating breast cancer prognosis
JP2009519710A (en) 2005-12-16 2009-05-21 ザ ボード オブ トラスティーズ オブ ザ レランド スタンフォード ジュニア ユニバーシティー Functional arrays for high-throughput characterization of gene expression regulatory elements
US20070167971A1 (en) 2006-01-17 2007-07-19 Raymond Huey Devices and methods for promoting the formation of blood clots in esophageal varices
AU2007217094A1 (en) 2006-02-17 2007-08-30 Janssen Pharmaceutica N.V. 11-phosphorous steroid derivatives useful as progesterone receptor modulators
DE102006054535A1 (en) 2006-11-15 2008-05-21 Bayer Schering Pharma Aktiengesellschaft Progesterone receptor antagonist
WO2008128783A2 (en) 2007-04-24 2008-10-30 Dsm Ip Assets B.V. Photochemical process for the preparation of a previtamin d
CA2596204C (en) 2007-08-07 2019-02-26 Historx, Inc. Method and system for determining an optimal dilution of a reagent
EP2075246A1 (en) * 2007-12-27 2009-07-01 M. J. Institute of Research A process for preparation of amorphous form of atorvastatin hemi-calcium salt
EA018974B9 (en) 2008-02-05 2014-04-30 Харбор Терапьютикс, Инк. Pharmaceutical solid state forms
TWI539953B (en) 2008-04-28 2016-07-01 瑞波若斯治療學公司 Compositions and methods for treating breast cancer
TW201002736A (en) 2008-04-28 2010-01-16 Repros Therapeutics Inc Compositions and methods for treating progesterone-dependent conditions
CN102365227B (en) 2009-03-27 2014-07-30 株式会社小松制作所 Fuel saving control device for working machine and fuel saving control method for working machine
US20110003753A1 (en) 2009-06-01 2011-01-06 Samuel Waxman Cancer Research Foundation COMPOSITIONS AND METHODS FOR DISRUPTING THE FUNCTION OF THE TRANSCRIPTIONAL REPRESSOR COMPONENT Sin3A-PAH2 DOMAIN TO INDUCE DIFFERENTIATION AND GROWTH INHIBITION IN BREAST CANCER
CA2768210C (en) 2009-07-15 2017-08-15 S*Bio Pte Ltd 9e-15-(2-pyrrolidin-1-yl-ethoxy)-7,12,25-trioxa-19,21,24-triaza- tetracyclo[18.3.1.1(2,5).1(14,18)]hexacosa-1(24),2,4,9,14,16,18(26),20,22-nonaene citrate salt
US20110293511A1 (en) 2009-09-29 2011-12-01 Terrance Grant Johns Specific binding proteins and uses thereof
EP2550288A1 (en) 2010-03-22 2013-01-30 Repros Therapeutics Inc. Compositions and methods for non-toxic delivery of antiprogestins
EP3702460A1 (en) 2010-11-12 2020-09-02 The General Hospital Corporation Polycomb-associated non-coding rnas
EP2655621B1 (en) 2010-12-20 2018-05-23 The General Hospital Corporation Polycomb-associated non-coding rnas
US20140079722A1 (en) 2011-03-09 2014-03-20 Centrose, Llc Extracellular targeted drug conjugates
CN103561744A (en) 2011-03-11 2014-02-05 细胞基因公司 Use of 3-(5-amino-2-methyl-4-oxoquinazolin-3(4H)-yl)piperidine-2-6-dione in treatment of immune-related and inflammatory diseases
WO2012141285A1 (en) 2011-04-15 2012-10-18 ジェイファーマ株式会社 Biomarker for breast cancer
US20130029953A1 (en) 2011-07-28 2013-01-31 Klaus Nickisch Progesterone antagonists
KR102009007B1 (en) 2011-10-04 2019-08-08 인비비스 파마슈티컬스 인코포레이티드 Methods and systems for identifying and treating anti-progestin sensitive tumors
WO2013086379A2 (en) 2011-12-08 2013-06-13 Fundacion Sales Methods and compositions for treating antiprogestin-resistant cancers
US20130338016A1 (en) 2012-04-17 2013-12-19 Vala Sciences, Inc. Method For Integrated Pathology Diagnosis And Digital Biomarker Pattern Analysis
MX2014013044A (en) 2012-04-27 2015-06-23 Univ Minnesota Breast cancer prognosis, prediction of progesterone receptor subtype and|prediction of response to antiprogestin treatment based on gene expression.
US20150241432A1 (en) 2012-07-24 2015-08-27 Cedar-Sinai Medical Center Novel method to detect resistance to chemotherapy in patients with lung cancer
US20140363425A1 (en) 2013-03-13 2014-12-11 J. Dinny Graham Systems and methods for identifying cancers having activated progesterone receptors
US9096641B2 (en) 2013-06-05 2015-08-04 Evestra, Inc. Imidazolyl progesterone antagonists
RU2016133175A (en) 2014-04-08 2018-05-08 Арно Терапьютикс, Инк. SYSTEMS AND METHODS FOR IDENTIFICATION OF RECEPTOR SUBTYPES TO PROGESTERON
US10786461B2 (en) 2014-11-17 2020-09-29 Context Biopharma Inc. Onapristone extended-release compositions and methods
MX2017012068A (en) 2015-03-23 2018-06-28 Evestra Inc Novel cytotoxic agents that preferentially target leukemia inhibitory factor (lif) for the treatment of malignancies and as new contraceptive agents.
BR112018005999A2 (en) 2015-09-25 2019-01-08 Context Biopharma Inc methods for the production of onapristone intermediates
KR20180113988A (en) 2015-12-15 2018-10-17 컨텍스트 바이오파마 인코포레이티드 Amorphous Ona Pristone Composition and Method of Manufacturing the Same
JP2019513706A (en) 2016-03-21 2019-05-30 コンテキスト・バイオファーマ・インコーポレイテッド Onapristone metabolite composition and method

Patent Citations (11)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5141961A (en) * 1991-06-27 1992-08-25 Richrdson-Vicks Inc. Process for solubilizing difficulty soluble pharmaceutical actives
US6143754A (en) * 1994-10-24 2000-11-07 Schering Aktiengesellschaft Competitive progesterone antagonist for demand-oriented female birth control
EP0803250A1 (en) * 1996-04-24 1997-10-29 American Home Food Products, Inc. Controlled release of steroids from sugar coatings
US6537584B1 (en) * 1999-11-12 2003-03-25 Macromed, Inc. Polymer blends that swell in an acidic environment and deswell in a basic environment
WO2006010097A2 (en) * 2004-07-09 2006-01-26 The Population Council, Inc. Sustained release compositions containing progesterone receptor modulators
WO2006111856A1 (en) * 2005-04-20 2006-10-26 Pfizer Limited Pyrazole derivatives as progesterone receptor antagonists
US20070166372A1 (en) * 2006-01-19 2007-07-19 Mai De Ltd. Preparation of solid coprecipitates of amorphous valsartan
US20120140790A1 (en) * 2009-12-15 2012-06-07 Ali Mir M Therapeutic Polymeric Nanoparticle Compositions with High Glass Transition Termperature or High Molecular Weight Copolymers
WO2012083017A2 (en) * 2010-12-16 2012-06-21 Celgene Corporation Controlled release oral dosage forms of poorly soluble drugs and uses thereof
WO2014093918A1 (en) * 2012-12-13 2014-06-19 Warsaw Orthopedic, Inc. Compositions and methods comprising polyethylene glycol and magnesium for treatment of neuronal injury
US9193757B2 (en) * 2013-03-12 2015-11-24 Arno Therapeutics, Inc. Onapristone polymorphic forms and methods of use

Non-Patent Citations (2)

* Cited by examiner, † Cited by third party
Title
See also references of EP3389632A4 *
SHI, S ET AL.: "Antigen retrieval immunohistochemistry under the influence of pH using monoclonal antibodies.", JOURNAL OF HISTOCHEMISTRY & CYTOCHEMISTRY., vol. 43, no. 2., 1995, pages 193 - 201, XP055391185 *

Also Published As

Publication number Publication date
AU2016370499B2 (en) 2022-06-30
CN108883067B (en) 2021-03-09
EP3389632A4 (en) 2019-11-06
JP2019503353A (en) 2019-02-07
CA3008422A1 (en) 2017-06-22
CN108883067A (en) 2018-11-23
US10548905B2 (en) 2020-02-04
AU2016370499A1 (en) 2018-07-12
KR20180113988A (en) 2018-10-17
US20200376004A1 (en) 2020-12-03
MX2018007154A (en) 2019-01-10
HK1255104A1 (en) 2019-08-02
US20170182065A1 (en) 2017-06-29
HK1256633A1 (en) 2019-09-27
EP3389632A1 (en) 2018-10-24

Similar Documents

Publication Publication Date Title
AU2016370499B2 (en) Amorphous onapristone compositions and methods of making the same
US8124603B2 (en) In vivo studies of crystalline forms of meloxicam
JP6577143B2 (en) Dosage form composition comprising an inhibitor of breton tyrosine kinase
AU2020419197B2 (en) Amorphous kinase inhibitor formulations and methods of use thereof
JP2018138594A (en) Onapristone polymorphic forms and methods of use
TW202334125A (en) Solid forms of a cdk4 inhibitor
TW201925207A (en) Salts of 4-amino-N-(1-((3-chloro-2-fluorophenyl)amino)-6-methylisoquinolin-5-yl)thieno[3,2-D]pyrimidine-7-carboxamide, and crystalline forms thereof
US8003672B2 (en) CB-1 receptor modulator formulations
TWI815820B (en) Solid forms of 2-(5-(4-(2-morpholinoethoxy)phenyl)pyridin-2-yl)-n-benzylacetamide
CN116514797A (en) Novel polymorphic forms of metoclopramide
NZ760233A (en) Compositions and methods for treatment of abnormal cell growth
KR20130130802A (en) Compositions and methods of using crystalline forms of wortmannin analogs
WO2021138483A1 (en) Amorphous kinase inhibitor formulations and methods of use thereof
EA045716B1 (en) COMPOSITION OF CONDENSED TRICYCLIC GAMA-AMINO ACID DERIVATIVES FOR TREATMENT AND/OR PREVENTION OF MECHANICAL PAIN AND ITS PREPARATION
BR122024012946A2 (en) COMPOUND, PHARMACEUTICAL COMPOSITION, USE OF A PHARMACEUTICAL COMPOSITION AND USE OF A COMPOUND

Legal Events

Date Code Title Description
121 Ep: the epo has been informed by wipo that ep was designated in this application

Ref document number: 16876503

Country of ref document: EP

Kind code of ref document: A1

WWE Wipo information: entry into national phase

Ref document number: MX/A/2018/007154

Country of ref document: MX

ENP Entry into the national phase

Ref document number: 3008422

Country of ref document: CA

WWE Wipo information: entry into national phase

Ref document number: 2018532190

Country of ref document: JP

NENP Non-entry into the national phase

Ref country code: DE

WWE Wipo information: entry into national phase

Ref document number: 1020187019175

Country of ref document: KR

ENP Entry into the national phase

Ref document number: 2016370499

Country of ref document: AU

Date of ref document: 20161213

Kind code of ref document: A

WWE Wipo information: entry into national phase

Ref document number: 2016876503

Country of ref document: EP

ENP Entry into the national phase

Ref document number: 2016876503

Country of ref document: EP

Effective date: 20180716