CA2790933A1 - Stable dosage forms of levomilnacipran - Google Patents
Stable dosage forms of levomilnacipran Download PDFInfo
- Publication number
- CA2790933A1 CA2790933A1 CA2790933A CA2790933A CA2790933A1 CA 2790933 A1 CA2790933 A1 CA 2790933A1 CA 2790933 A CA2790933 A CA 2790933A CA 2790933 A CA2790933 A CA 2790933A CA 2790933 A1 CA2790933 A1 CA 2790933A1
- Authority
- CA
- Canada
- Prior art keywords
- dosage form
- stable dosage
- levomilnacipran
- stable
- less
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Abandoned
Links
- 239000002552 dosage form Substances 0.000 title claims abstract description 500
- GJJFMKBJSRMPLA-HIFRSBDPSA-N (1R,2S)-2-(aminomethyl)-N,N-diethyl-1-phenyl-1-cyclopropanecarboxamide Chemical compound C=1C=CC=CC=1[C@@]1(C(=O)N(CC)CC)C[C@@H]1CN GJJFMKBJSRMPLA-HIFRSBDPSA-N 0.000 title claims abstract description 187
- 229960000685 levomilnacipran Drugs 0.000 title claims abstract description 186
- 238000000034 method Methods 0.000 claims abstract description 45
- 150000003839 salts Chemical class 0.000 claims abstract description 32
- 238000004090 dissolution Methods 0.000 claims description 116
- 238000000634 powder X-ray diffraction Methods 0.000 claims description 45
- 230000000181 anti-adherent effect Effects 0.000 claims description 37
- 239000003911 antiadherent Substances 0.000 claims description 37
- 239000011230 binding agent Substances 0.000 claims description 35
- 239000003795 chemical substances by application Substances 0.000 claims description 35
- 239000004480 active ingredient Substances 0.000 claims description 34
- 239000000314 lubricant Substances 0.000 claims description 33
- 239000000758 substrate Substances 0.000 claims description 33
- LFQSCWFLJHTTHZ-UHFFFAOYSA-N Ethanol Chemical compound CCO LFQSCWFLJHTTHZ-UHFFFAOYSA-N 0.000 claims description 23
- 239000000945 filler Substances 0.000 claims description 23
- 208000024714 major depressive disease Diseases 0.000 claims description 21
- 239000004014 plasticizer Substances 0.000 claims description 20
- QQZOPKMRPOGIEB-UHFFFAOYSA-N 2-Oxohexane Chemical compound CCCCC(C)=O QQZOPKMRPOGIEB-UHFFFAOYSA-N 0.000 claims description 16
- 238000002441 X-ray diffraction Methods 0.000 claims description 14
- 239000006186 oral dosage form Substances 0.000 claims description 14
- 229960000935 dehydrated alcohol Drugs 0.000 claims description 12
- 239000012729 immediate-release (IR) formulation Substances 0.000 claims description 11
- 230000008569 process Effects 0.000 abstract description 10
- 238000002360 preparation method Methods 0.000 abstract description 4
- XLYOFNOQVPJJNP-UHFFFAOYSA-N water Substances O XLYOFNOQVPJJNP-UHFFFAOYSA-N 0.000 description 56
- 239000008367 deionised water Substances 0.000 description 44
- 229910021641 deionized water Inorganic materials 0.000 description 44
- 239000011324 bead Substances 0.000 description 36
- QZAYGJVTTNCVMB-UHFFFAOYSA-N serotonin Chemical compound C1=C(O)C=C2C(CCN)=CNC2=C1 QZAYGJVTTNCVMB-UHFFFAOYSA-N 0.000 description 28
- 239000000203 mixture Substances 0.000 description 27
- 239000002904 solvent Substances 0.000 description 27
- 238000003860 storage Methods 0.000 description 26
- 239000002775 capsule Substances 0.000 description 25
- 239000008187 granular material Substances 0.000 description 25
- 235000002639 sodium chloride Nutrition 0.000 description 25
- 239000001856 Ethyl cellulose Substances 0.000 description 21
- ZZSNKZQZMQGXPY-UHFFFAOYSA-N Ethyl cellulose Chemical compound CCOCC1OC(OC)C(OCC)C(OCC)C1OC1C(O)C(O)C(OC)C(CO)O1 ZZSNKZQZMQGXPY-UHFFFAOYSA-N 0.000 description 21
- 235000019325 ethyl cellulose Nutrition 0.000 description 21
- 229920001249 ethyl cellulose Polymers 0.000 description 21
- 239000002274 desiccant Substances 0.000 description 19
- 238000013268 sustained release Methods 0.000 description 17
- 239000012730 sustained-release form Substances 0.000 description 17
- 235000010979 hydroxypropyl methyl cellulose Nutrition 0.000 description 16
- 229920003088 hydroxypropyl methyl cellulose Polymers 0.000 description 16
- SFLSHLFXELFNJZ-QMMMGPOBSA-N (-)-norepinephrine Chemical compound NC[C@H](O)C1=CC=C(O)C(O)=C1 SFLSHLFXELFNJZ-QMMMGPOBSA-N 0.000 description 15
- 229960002748 norepinephrine Drugs 0.000 description 15
- SFLSHLFXELFNJZ-UHFFFAOYSA-N norepinephrine Natural products NCC(O)C1=CC=C(O)C(O)=C1 SFLSHLFXELFNJZ-UHFFFAOYSA-N 0.000 description 15
- 230000036470 plasma concentration Effects 0.000 description 15
- 239000000454 talc Substances 0.000 description 14
- 229910052623 talc Inorganic materials 0.000 description 14
- 208000037265 diseases, disorders, signs and symptoms Diseases 0.000 description 13
- 229920000036 polyvinylpyrrolidone Polymers 0.000 description 12
- 235000013855 polyvinylpyrrolidone Nutrition 0.000 description 12
- DOOTYTYQINUNNV-UHFFFAOYSA-N Triethyl citrate Chemical compound CCOC(=O)CC(O)(C(=O)OCC)CC(=O)OCC DOOTYTYQINUNNV-UHFFFAOYSA-N 0.000 description 10
- 239000003814 drug Substances 0.000 description 10
- 238000009472 formulation Methods 0.000 description 10
- 230000005764 inhibitory process Effects 0.000 description 10
- 239000001069 triethyl citrate Substances 0.000 description 10
- VMYFZRTXGLUXMZ-UHFFFAOYSA-N triethyl citrate Natural products CCOC(=O)C(O)(C(=O)OCC)C(=O)OCC VMYFZRTXGLUXMZ-UHFFFAOYSA-N 0.000 description 10
- 235000013769 triethyl citrate Nutrition 0.000 description 10
- WHNWPMSKXPGLAX-UHFFFAOYSA-N N-Vinyl-2-pyrrolidone Chemical compound C=CN1CCCC1=O WHNWPMSKXPGLAX-UHFFFAOYSA-N 0.000 description 9
- 229920001688 coating polymer Polymers 0.000 description 9
- 229940079593 drug Drugs 0.000 description 9
- 239000011162 core material Substances 0.000 description 8
- 210000002381 plasma Anatomy 0.000 description 8
- 201000010099 disease Diseases 0.000 description 7
- 208000035475 disorder Diseases 0.000 description 6
- 208000019901 Anxiety disease Diseases 0.000 description 5
- 229920003081 Povidone K 30 Polymers 0.000 description 5
- 239000012530 fluid Substances 0.000 description 5
- 239000007903 gelatin capsule Substances 0.000 description 5
- 239000012535 impurity Substances 0.000 description 5
- 238000001727 in vivo Methods 0.000 description 5
- 239000008186 active pharmaceutical agent Substances 0.000 description 4
- 239000011248 coating agent Substances 0.000 description 4
- 238000000576 coating method Methods 0.000 description 4
- 229940076279 serotonin Drugs 0.000 description 4
- 239000003775 serotonin noradrenalin reuptake inhibitor Substances 0.000 description 4
- 239000007787 solid Substances 0.000 description 4
- 239000000126 substance Substances 0.000 description 4
- NIXOWILDQLNWCW-UHFFFAOYSA-N 2-Propenoic acid Natural products OC(=O)C=C NIXOWILDQLNWCW-UHFFFAOYSA-N 0.000 description 3
- 229910016523 CuKa Inorganic materials 0.000 description 3
- 208000020401 Depressive disease Diseases 0.000 description 3
- 239000002202 Polyethylene glycol Substances 0.000 description 3
- DNIAPMSPPWPWGF-UHFFFAOYSA-N Propylene glycol Chemical compound CC(O)CO DNIAPMSPPWPWGF-UHFFFAOYSA-N 0.000 description 3
- 229920002125 Sokalan® Polymers 0.000 description 3
- 229920002472 Starch Polymers 0.000 description 3
- 239000013543 active substance Substances 0.000 description 3
- XAGFODPZIPBFFR-UHFFFAOYSA-N aluminium Chemical compound [Al] XAGFODPZIPBFFR-UHFFFAOYSA-N 0.000 description 3
- 229910052782 aluminium Inorganic materials 0.000 description 3
- 238000004458 analytical method Methods 0.000 description 3
- 230000036506 anxiety Effects 0.000 description 3
- 239000008199 coating composition Substances 0.000 description 3
- 238000007405 data analysis Methods 0.000 description 3
- 238000013480 data collection Methods 0.000 description 3
- 239000008380 degradant Substances 0.000 description 3
- 238000002050 diffraction method Methods 0.000 description 3
- 238000004519 manufacturing process Methods 0.000 description 3
- 239000004531 microgranule Substances 0.000 description 3
- 239000000546 pharmaceutical excipient Substances 0.000 description 3
- 229920001223 polyethylene glycol Polymers 0.000 description 3
- 239000001267 polyvinylpyrrolidone Substances 0.000 description 3
- 230000005855 radiation Effects 0.000 description 3
- 235000019698 starch Nutrition 0.000 description 3
- 230000001225 therapeutic effect Effects 0.000 description 3
- XNCDYJFPRPDERF-NQQJLSKUSA-N (1s,2r)-2-(aminomethyl)-n,n-diethyl-1-phenylcyclopropane-1-carboxamide;hydrochloride Chemical compound Cl.C=1C=CC=CC=1[C@]1(C(=O)N(CC)CC)C[C@H]1CN XNCDYJFPRPDERF-NQQJLSKUSA-N 0.000 description 2
- VBICKXHEKHSIBG-UHFFFAOYSA-N 1-monostearoylglycerol Chemical compound CCCCCCCCCCCCCCCCCC(=O)OCC(O)CO VBICKXHEKHSIBG-UHFFFAOYSA-N 0.000 description 2
- SMZOUWXMTYCWNB-UHFFFAOYSA-N 2-(2-methoxy-5-methylphenyl)ethanamine Chemical compound COC1=CC=C(C)C=C1CCN SMZOUWXMTYCWNB-UHFFFAOYSA-N 0.000 description 2
- 229920002126 Acrylic acid copolymer Polymers 0.000 description 2
- GUBGYTABKSRVRQ-XLOQQCSPSA-N Alpha-Lactose Chemical compound O[C@@H]1[C@@H](O)[C@@H](O)[C@@H](CO)O[C@H]1O[C@@H]1[C@@H](CO)O[C@H](O)[C@H](O)[C@H]1O GUBGYTABKSRVRQ-XLOQQCSPSA-N 0.000 description 2
- FBPFZTCFMRRESA-FSIIMWSLSA-N D-Glucitol Natural products OC[C@H](O)[C@H](O)[C@@H](O)[C@H](O)CO FBPFZTCFMRRESA-FSIIMWSLSA-N 0.000 description 2
- FBPFZTCFMRRESA-JGWLITMVSA-N D-glucitol Chemical compound OC[C@H](O)[C@@H](O)[C@H](O)[C@H](O)CO FBPFZTCFMRRESA-JGWLITMVSA-N 0.000 description 2
- NIQCNGHVCWTJSM-UHFFFAOYSA-N Dimethyl phthalate Chemical compound COC(=O)C1=CC=CC=C1C(=O)OC NIQCNGHVCWTJSM-UHFFFAOYSA-N 0.000 description 2
- 108010010803 Gelatin Proteins 0.000 description 2
- WQZGKKKJIJFFOK-GASJEMHNSA-N Glucose Natural products OC[C@H]1OC(O)[C@H](O)[C@@H](O)[C@@H]1O WQZGKKKJIJFFOK-GASJEMHNSA-N 0.000 description 2
- 229920002153 Hydroxypropyl cellulose Polymers 0.000 description 2
- GUBGYTABKSRVRQ-QKKXKWKRSA-N Lactose Natural products OC[C@H]1O[C@@H](O[C@H]2[C@H](O)[C@@H](O)C(O)O[C@@H]2CO)[C@H](O)[C@@H](O)[C@H]1O GUBGYTABKSRVRQ-QKKXKWKRSA-N 0.000 description 2
- 241000124008 Mammalia Species 0.000 description 2
- CERQOIWHTDAKMF-UHFFFAOYSA-N Methacrylic acid Chemical class CC(=C)C(O)=O CERQOIWHTDAKMF-UHFFFAOYSA-N 0.000 description 2
- BAPJBEWLBFYGME-UHFFFAOYSA-N Methyl acrylate Chemical compound COC(=O)C=C BAPJBEWLBFYGME-UHFFFAOYSA-N 0.000 description 2
- 229920000881 Modified starch Polymers 0.000 description 2
- 208000002193 Pain Diseases 0.000 description 2
- 229940121991 Serotonin and norepinephrine reuptake inhibitor Drugs 0.000 description 2
- FAPWRFPIFSIZLT-UHFFFAOYSA-M Sodium chloride Chemical compound [Na+].[Cl-] FAPWRFPIFSIZLT-UHFFFAOYSA-M 0.000 description 2
- CZMRCDWAGMRECN-UGDNZRGBSA-N Sucrose Chemical compound O[C@H]1[C@H](O)[C@@H](CO)O[C@@]1(CO)O[C@@H]1[C@H](O)[C@@H](O)[C@H](O)[C@@H](CO)O1 CZMRCDWAGMRECN-UGDNZRGBSA-N 0.000 description 2
- 229930006000 Sucrose Natural products 0.000 description 2
- ZFOZVQLOBQUTQQ-UHFFFAOYSA-N Tributyl citrate Chemical compound CCCCOC(=O)CC(O)(C(=O)OCCCC)CC(=O)OCCCC ZFOZVQLOBQUTQQ-UHFFFAOYSA-N 0.000 description 2
- 239000000654 additive Substances 0.000 description 2
- WQZGKKKJIJFFOK-VFUOTHLCSA-N beta-D-glucose Chemical compound OC[C@H]1O[C@@H](O)[C@H](O)[C@@H](O)[C@@H]1O WQZGKKKJIJFFOK-VFUOTHLCSA-N 0.000 description 2
- OSGAYBCDTDRGGQ-UHFFFAOYSA-L calcium sulfate Chemical compound [Ca+2].[O-]S([O-])(=O)=O OSGAYBCDTDRGGQ-UHFFFAOYSA-L 0.000 description 2
- 235000010980 cellulose Nutrition 0.000 description 2
- 229920002678 cellulose Polymers 0.000 description 2
- 239000001913 cellulose Substances 0.000 description 2
- 229920002301 cellulose acetate Polymers 0.000 description 2
- 229920001577 copolymer Polymers 0.000 description 2
- DOIRQSBPFJWKBE-UHFFFAOYSA-N dibutyl phthalate Chemical compound CCCCOC(=O)C1=CC=CC=C1C(=O)OCCCC DOIRQSBPFJWKBE-UHFFFAOYSA-N 0.000 description 2
- RBLGLDWTCZMLRW-UHFFFAOYSA-K dicalcium;phosphate;dihydrate Chemical compound O.O.[Ca+2].[Ca+2].[O-]P([O-])([O-])=O RBLGLDWTCZMLRW-UHFFFAOYSA-K 0.000 description 2
- FLKPEMZONWLCSK-UHFFFAOYSA-N diethyl phthalate Chemical compound CCOC(=O)C1=CC=CC=C1C(=O)OCC FLKPEMZONWLCSK-UHFFFAOYSA-N 0.000 description 2
- 239000006185 dispersion Substances 0.000 description 2
- 229960004756 ethanol Drugs 0.000 description 2
- -1 for example Substances 0.000 description 2
- 230000002496 gastric effect Effects 0.000 description 2
- 229920000159 gelatin Polymers 0.000 description 2
- 239000008273 gelatin Substances 0.000 description 2
- 235000019322 gelatine Nutrition 0.000 description 2
- 235000011852 gelatine desserts Nutrition 0.000 description 2
- 235000010977 hydroxypropyl cellulose Nutrition 0.000 description 2
- 239000001863 hydroxypropyl cellulose Substances 0.000 description 2
- 239000001866 hydroxypropyl methyl cellulose Substances 0.000 description 2
- UFVKGYZPFZQRLF-UHFFFAOYSA-N hydroxypropyl methyl cellulose Chemical compound OC1C(O)C(OC)OC(CO)C1OC1C(O)C(O)C(OC2C(C(O)C(OC3C(C(O)C(O)C(CO)O3)O)C(CO)O2)O)C(CO)O1 UFVKGYZPFZQRLF-UHFFFAOYSA-N 0.000 description 2
- 230000002401 inhibitory effect Effects 0.000 description 2
- 230000000968 intestinal effect Effects 0.000 description 2
- 239000008101 lactose Substances 0.000 description 2
- 229960001926 levomilnacipran hydrochloride Drugs 0.000 description 2
- 238000011068 loading method Methods 0.000 description 2
- HQKMJHAJHXVSDF-UHFFFAOYSA-L magnesium stearate Chemical compound [Mg+2].CCCCCCCCCCCCCCCCCC([O-])=O.CCCCCCCCCCCCCCCCCC([O-])=O HQKMJHAJHXVSDF-UHFFFAOYSA-L 0.000 description 2
- 229920003145 methacrylic acid copolymer Polymers 0.000 description 2
- 238000011002 quantification Methods 0.000 description 2
- 230000002441 reversible effect Effects 0.000 description 2
- 239000007909 solid dosage form Substances 0.000 description 2
- 239000000600 sorbitol Substances 0.000 description 2
- 235000010356 sorbitol Nutrition 0.000 description 2
- 239000008107 starch Substances 0.000 description 2
- 239000005720 sucrose Substances 0.000 description 2
- 208000024891 symptom Diseases 0.000 description 2
- 239000003826 tablet Substances 0.000 description 2
- URAYPUMNDPQOKB-UHFFFAOYSA-N triacetin Chemical compound CC(=O)OCC(OC(C)=O)COC(C)=O URAYPUMNDPQOKB-UHFFFAOYSA-N 0.000 description 2
- 239000001993 wax Substances 0.000 description 2
- SERLAGPUMNYUCK-DCUALPFSSA-N 1-O-alpha-D-glucopyranosyl-D-mannitol Chemical compound OC[C@@H](O)[C@@H](O)[C@H](O)[C@H](O)CO[C@H]1O[C@H](CO)[C@@H](O)[C@H](O)[C@H]1O SERLAGPUMNYUCK-DCUALPFSSA-N 0.000 description 1
- OKMWKBLSFKFYGZ-UHFFFAOYSA-N 1-behenoylglycerol Chemical compound CCCCCCCCCCCCCCCCCCCCCC(=O)OCC(O)CO OKMWKBLSFKFYGZ-UHFFFAOYSA-N 0.000 description 1
- IXPNQXFRVYWDDI-UHFFFAOYSA-N 1-methyl-2,4-dioxo-1,3-diazinane-5-carboximidamide Chemical compound CN1CC(C(N)=N)C(=O)NC1=O IXPNQXFRVYWDDI-UHFFFAOYSA-N 0.000 description 1
- 239000005995 Aluminium silicate Substances 0.000 description 1
- 229920000856 Amylose Polymers 0.000 description 1
- 241000416162 Astragalus gummifer Species 0.000 description 1
- 229920000623 Cellulose acetate phthalate Polymers 0.000 description 1
- PTHCMJGKKRQCBF-UHFFFAOYSA-N Cellulose, microcrystalline Chemical compound OC1C(O)C(OC)OC(CO)C1OC1C(O)C(O)C(OC)C(CO)O1 PTHCMJGKKRQCBF-UHFFFAOYSA-N 0.000 description 1
- 229920001661 Chitosan Polymers 0.000 description 1
- 208000028698 Cognitive impairment Diseases 0.000 description 1
- FBPFZTCFMRRESA-KVTDHHQDSA-N D-Mannitol Chemical compound OC[C@@H](O)[C@@H](O)[C@H](O)[C@H](O)CO FBPFZTCFMRRESA-KVTDHHQDSA-N 0.000 description 1
- PYGXAGIECVVIOZ-UHFFFAOYSA-N Dibutyl decanedioate Chemical compound CCCCOC(=O)CCCCCCCCC(=O)OCCCC PYGXAGIECVVIOZ-UHFFFAOYSA-N 0.000 description 1
- 208000010228 Erectile Dysfunction Diseases 0.000 description 1
- JIGUQPWFLRLWPJ-UHFFFAOYSA-N Ethyl acrylate Chemical compound CCOC(=O)C=C JIGUQPWFLRLWPJ-UHFFFAOYSA-N 0.000 description 1
- 206010017788 Gastric haemorrhage Diseases 0.000 description 1
- 208000011688 Generalised anxiety disease Diseases 0.000 description 1
- 229920002907 Guar gum Polymers 0.000 description 1
- 239000004354 Hydroxyethyl cellulose Substances 0.000 description 1
- 229920000663 Hydroxyethyl cellulose Polymers 0.000 description 1
- 208000031226 Hyperlipidaemia Diseases 0.000 description 1
- 240000007472 Leucaena leucocephala Species 0.000 description 1
- 235000010643 Leucaena leucocephala Nutrition 0.000 description 1
- 229930195725 Mannitol Natural products 0.000 description 1
- VVQNEPGJFQJSBK-UHFFFAOYSA-N Methyl methacrylate Chemical compound COC(=O)C(C)=C VVQNEPGJFQJSBK-UHFFFAOYSA-N 0.000 description 1
- 229920000168 Microcrystalline cellulose Polymers 0.000 description 1
- 206010028813 Nausea Diseases 0.000 description 1
- 229920003171 Poly (ethylene oxide) Polymers 0.000 description 1
- 229920002845 Poly(methacrylic acid) Polymers 0.000 description 1
- 229920000148 Polycarbophil calcium Polymers 0.000 description 1
- 239000004372 Polyvinyl alcohol Substances 0.000 description 1
- 201000001880 Sexual dysfunction Diseases 0.000 description 1
- 229920001800 Shellac Polymers 0.000 description 1
- VYPSYNLAJGMNEJ-UHFFFAOYSA-N Silicium dioxide Chemical compound O=[Si]=O VYPSYNLAJGMNEJ-UHFFFAOYSA-N 0.000 description 1
- 208000032140 Sleepiness Diseases 0.000 description 1
- 206010041349 Somnolence Diseases 0.000 description 1
- 235000021355 Stearic acid Nutrition 0.000 description 1
- GWEVSGVZZGPLCZ-UHFFFAOYSA-N Titan oxide Chemical compound O=[Ti]=O GWEVSGVZZGPLCZ-UHFFFAOYSA-N 0.000 description 1
- 229920001615 Tragacanth Polymers 0.000 description 1
- XTXRWKRVRITETP-UHFFFAOYSA-N Vinyl acetate Chemical compound CC(=O)OC=C XTXRWKRVRITETP-UHFFFAOYSA-N 0.000 description 1
- 206010047700 Vomiting Diseases 0.000 description 1
- 229920002494 Zein Polymers 0.000 description 1
- DPXJVFZANSGRMM-UHFFFAOYSA-N acetic acid;2,3,4,5,6-pentahydroxyhexanal;sodium Chemical compound [Na].CC(O)=O.OCC(O)C(O)C(O)C(O)C=O DPXJVFZANSGRMM-UHFFFAOYSA-N 0.000 description 1
- 230000001154 acute effect Effects 0.000 description 1
- 230000000996 additive effect Effects 0.000 description 1
- 230000002411 adverse Effects 0.000 description 1
- 230000004075 alteration Effects 0.000 description 1
- 235000012211 aluminium silicate Nutrition 0.000 description 1
- SNAAJJQQZSMGQD-UHFFFAOYSA-N aluminum magnesium Chemical compound [Mg].[Al] SNAAJJQQZSMGQD-UHFFFAOYSA-N 0.000 description 1
- 229920003144 amino alkyl methacrylate copolymer Polymers 0.000 description 1
- 208000025748 atypical depressive disease Diseases 0.000 description 1
- 230000008901 benefit Effects 0.000 description 1
- 230000008512 biological response Effects 0.000 description 1
- 210000004369 blood Anatomy 0.000 description 1
- 239000008280 blood Substances 0.000 description 1
- 230000037058 blood plasma level Effects 0.000 description 1
- CJZGTCYPCWQAJB-UHFFFAOYSA-L calcium stearate Chemical compound [Ca+2].CCCCCCCCCCCCCCCCCC([O-])=O.CCCCCCCCCCCCCCCCCC([O-])=O CJZGTCYPCWQAJB-UHFFFAOYSA-L 0.000 description 1
- 239000008116 calcium stearate Substances 0.000 description 1
- 235000013539 calcium stearate Nutrition 0.000 description 1
- 239000007894 caplet Substances 0.000 description 1
- 229960001631 carbomer Drugs 0.000 description 1
- 229920003123 carboxymethyl cellulose sodium Polymers 0.000 description 1
- 229940063834 carboxymethylcellulose sodium Drugs 0.000 description 1
- 239000004359 castor oil Substances 0.000 description 1
- 235000019438 castor oil Nutrition 0.000 description 1
- 229940081734 cellulose acetate phthalate Drugs 0.000 description 1
- 238000004587 chromatography analysis Methods 0.000 description 1
- 208000010877 cognitive disease Diseases 0.000 description 1
- 239000003086 colorant Substances 0.000 description 1
- 229920006237 degradable polymer Polymers 0.000 description 1
- 230000003111 delayed effect Effects 0.000 description 1
- 238000001514 detection method Methods 0.000 description 1
- 239000008121 dextrose Substances 0.000 description 1
- 206010012601 diabetes mellitus Diseases 0.000 description 1
- 229940099371 diacetylated monoglycerides Drugs 0.000 description 1
- FBSAITBEAPNWJG-UHFFFAOYSA-N dimethyl phthalate Natural products CC(=O)OC1=CC=CC=C1OC(C)=O FBSAITBEAPNWJG-UHFFFAOYSA-N 0.000 description 1
- 229960001826 dimethylphthalate Drugs 0.000 description 1
- 208000024732 dysthymic disease Diseases 0.000 description 1
- 230000000694 effects Effects 0.000 description 1
- LUJQXGBDWAGQHS-UHFFFAOYSA-N ethenyl acetate;phthalic acid Chemical compound CC(=O)OC=C.OC(=O)C1=CC=CC=C1C(O)=O LUJQXGBDWAGQHS-UHFFFAOYSA-N 0.000 description 1
- SUPCQIBBMFXVTL-UHFFFAOYSA-N ethyl 2-methylprop-2-enoate Chemical compound CCOC(=O)C(C)=C SUPCQIBBMFXVTL-UHFFFAOYSA-N 0.000 description 1
- MVPICKVDHDWCJQ-UHFFFAOYSA-N ethyl 3-pyrrolidin-1-ylpropanoate Chemical compound CCOC(=O)CCN1CCCC1 MVPICKVDHDWCJQ-UHFFFAOYSA-N 0.000 description 1
- 239000005038 ethylene vinyl acetate Substances 0.000 description 1
- 238000013265 extended release Methods 0.000 description 1
- 238000000605 extraction Methods 0.000 description 1
- 238000011049 filling Methods 0.000 description 1
- 239000007897 gelcap Substances 0.000 description 1
- 208000029364 generalized anxiety disease Diseases 0.000 description 1
- 239000008103 glucose Substances 0.000 description 1
- YQEMORVAKMFKLG-UHFFFAOYSA-N glycerine monostearate Natural products CCCCCCCCCCCCCCCCCC(=O)OC(CO)CO YQEMORVAKMFKLG-UHFFFAOYSA-N 0.000 description 1
- SVUQHVRAGMNPLW-UHFFFAOYSA-N glycerol monostearate Natural products CCCCCCCCCCCCCCCCC(=O)OCC(O)CO SVUQHVRAGMNPLW-UHFFFAOYSA-N 0.000 description 1
- ZEMPKEQAKRGZGQ-XOQCFJPHSA-N glycerol triricinoleate Natural products CCCCCC[C@@H](O)CC=CCCCCCCCC(=O)OC[C@@H](COC(=O)CCCCCCCC=CC[C@@H](O)CCCCCC)OC(=O)CCCCCCCC=CC[C@H](O)CCCCCC ZEMPKEQAKRGZGQ-XOQCFJPHSA-N 0.000 description 1
- 239000001087 glyceryl triacetate Substances 0.000 description 1
- 235000013773 glyceryl triacetate Nutrition 0.000 description 1
- 239000000665 guar gum Substances 0.000 description 1
- 235000010417 guar gum Nutrition 0.000 description 1
- 229960002154 guar gum Drugs 0.000 description 1
- 229920000591 gum Polymers 0.000 description 1
- 238000004128 high performance liquid chromatography Methods 0.000 description 1
- 235000019447 hydroxyethyl cellulose Nutrition 0.000 description 1
- 229920003063 hydroxymethyl cellulose Polymers 0.000 description 1
- 229940031574 hydroxymethyl cellulose Drugs 0.000 description 1
- 229920003132 hydroxypropyl methylcellulose phthalate Polymers 0.000 description 1
- 229940031704 hydroxypropyl methylcellulose phthalate Drugs 0.000 description 1
- 229920000639 hydroxypropylmethylcellulose acetate succinate Polymers 0.000 description 1
- 201000001881 impotence Diseases 0.000 description 1
- 239000003112 inhibitor Substances 0.000 description 1
- 239000002050 international nonproprietary name Substances 0.000 description 1
- 239000000905 isomalt Substances 0.000 description 1
- 235000010439 isomalt Nutrition 0.000 description 1
- HPIGCVXMBGOWTF-UHFFFAOYSA-N isomaltol Natural products CC(=O)C=1OC=CC=1O HPIGCVXMBGOWTF-UHFFFAOYSA-N 0.000 description 1
- 239000010977 jade Substances 0.000 description 1
- NLYAJNPCOHFWQQ-UHFFFAOYSA-N kaolin Chemical compound O.O.O=[Al]O[Si](=O)O[Si](=O)O[Al]=O NLYAJNPCOHFWQQ-UHFFFAOYSA-N 0.000 description 1
- 230000000670 limiting effect Effects 0.000 description 1
- 239000007788 liquid Substances 0.000 description 1
- 239000007937 lozenge Substances 0.000 description 1
- 235000019359 magnesium stearate Nutrition 0.000 description 1
- 239000000594 mannitol Substances 0.000 description 1
- 235000010355 mannitol Nutrition 0.000 description 1
- 239000000463 material Substances 0.000 description 1
- 238000005259 measurement Methods 0.000 description 1
- 201000003995 melancholia Diseases 0.000 description 1
- 125000005395 methacrylic acid group Chemical group 0.000 description 1
- 229920000609 methyl cellulose Polymers 0.000 description 1
- 235000010981 methylcellulose Nutrition 0.000 description 1
- 239000001923 methylcellulose Substances 0.000 description 1
- 235000019813 microcrystalline cellulose Nutrition 0.000 description 1
- 239000008108 microcrystalline cellulose Substances 0.000 description 1
- 229940016286 microcrystalline cellulose Drugs 0.000 description 1
- 239000002480 mineral oil Substances 0.000 description 1
- 235000010446 mineral oil Nutrition 0.000 description 1
- 230000004048 modification Effects 0.000 description 1
- 238000012986 modification Methods 0.000 description 1
- 230000008693 nausea Effects 0.000 description 1
- 208000004296 neuralgia Diseases 0.000 description 1
- 208000021722 neuropathic pain Diseases 0.000 description 1
- QIQXTHQIDYTFRH-UHFFFAOYSA-N octadecanoic acid Chemical compound CCCCCCCCCCCCCCCCCC(O)=O QIQXTHQIDYTFRH-UHFFFAOYSA-N 0.000 description 1
- OQCDKBAXFALNLD-UHFFFAOYSA-N octadecanoic acid Natural products CCCCCCCC(C)CCCCCCCCC(O)=O OQCDKBAXFALNLD-UHFFFAOYSA-N 0.000 description 1
- 235000010987 pectin Nutrition 0.000 description 1
- 239000001814 pectin Substances 0.000 description 1
- 229920001277 pectin Polymers 0.000 description 1
- PNJWIWWMYCMZRO-UHFFFAOYSA-N pent‐4‐en‐2‐one Natural products CC(=O)CC=C PNJWIWWMYCMZRO-UHFFFAOYSA-N 0.000 description 1
- 239000000049 pigment Substances 0.000 description 1
- 229920001200 poly(ethylene-vinyl acetate) Polymers 0.000 description 1
- 239000004584 polyacrylic acid Substances 0.000 description 1
- 229920001281 polyalkylene Polymers 0.000 description 1
- 229950005134 polycarbophil Drugs 0.000 description 1
- 229920000642 polymer Polymers 0.000 description 1
- 229920005862 polyol Polymers 0.000 description 1
- 150000003077 polyols Chemical class 0.000 description 1
- 229920002451 polyvinyl alcohol Polymers 0.000 description 1
- 230000003389 potentiating effect Effects 0.000 description 1
- 239000000843 powder Substances 0.000 description 1
- 229960004063 propylene glycol Drugs 0.000 description 1
- 230000009257 reactivity Effects 0.000 description 1
- 229920005989 resin Polymers 0.000 description 1
- 239000011347 resin Substances 0.000 description 1
- 238000004007 reversed phase HPLC Methods 0.000 description 1
- 230000035945 sensitivity Effects 0.000 description 1
- 231100000872 sexual dysfunction Toxicity 0.000 description 1
- 239000004208 shellac Substances 0.000 description 1
- 229940113147 shellac Drugs 0.000 description 1
- ZLGIYFNHBLSMPS-ATJNOEHPSA-N shellac Chemical compound OCCCCCC(O)C(O)CCCCCCCC(O)=O.C1C23[C@H](C(O)=O)CCC2[C@](C)(CO)[C@@H]1C(C(O)=O)=C[C@@H]3O ZLGIYFNHBLSMPS-ATJNOEHPSA-N 0.000 description 1
- 235000013874 shellac Nutrition 0.000 description 1
- 208000019116 sleep disease Diseases 0.000 description 1
- 235000010413 sodium alginate Nutrition 0.000 description 1
- 239000000661 sodium alginate Substances 0.000 description 1
- 229940005550 sodium alginate Drugs 0.000 description 1
- 239000011780 sodium chloride Substances 0.000 description 1
- 229940045902 sodium stearyl fumarate Drugs 0.000 description 1
- 239000003381 stabilizer Substances 0.000 description 1
- 239000008117 stearic acid Substances 0.000 description 1
- 229920001059 synthetic polymer Polymers 0.000 description 1
- 238000004885 tandem mass spectrometry Methods 0.000 description 1
- 238000011287 therapeutic dose Methods 0.000 description 1
- OGIDPMRJRNCKJF-UHFFFAOYSA-N titanium oxide Inorganic materials [Ti]=O OGIDPMRJRNCKJF-UHFFFAOYSA-N 0.000 description 1
- 235000010487 tragacanth Nutrition 0.000 description 1
- 239000000196 tragacanth Substances 0.000 description 1
- 229940116362 tragacanth Drugs 0.000 description 1
- 229960002622 triacetin Drugs 0.000 description 1
- WEAPVABOECTMGR-UHFFFAOYSA-N triethyl 2-acetyloxypropane-1,2,3-tricarboxylate Chemical compound CCOC(=O)CC(C(=O)OCC)(OC(C)=O)CC(=O)OCC WEAPVABOECTMGR-UHFFFAOYSA-N 0.000 description 1
- 125000005591 trimellitate group Chemical group 0.000 description 1
- 238000000825 ultraviolet detection Methods 0.000 description 1
- 229920006163 vinyl copolymer Polymers 0.000 description 1
- 229920002554 vinyl polymer Polymers 0.000 description 1
- 230000008673 vomiting Effects 0.000 description 1
- 239000005019 zein Substances 0.000 description 1
- 229940093612 zein Drugs 0.000 description 1
Classifications
-
- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D209/00—Heterocyclic compounds containing five-membered rings, condensed with other rings, with one nitrogen atom as the only ring hetero atom
- C07D209/02—Heterocyclic compounds containing five-membered rings, condensed with other rings, with one nitrogen atom as the only ring hetero atom condensed with one carbocyclic ring
- C07D209/52—Heterocyclic compounds containing five-membered rings, condensed with other rings, with one nitrogen atom as the only ring hetero atom condensed with one carbocyclic ring condensed with a ring other than six-membered
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K31/00—Medicinal preparations containing organic active ingredients
- A61K31/16—Amides, e.g. hydroxamic acids
- A61K31/165—Amides, e.g. hydroxamic acids having aromatic rings, e.g. colchicine, atenolol, progabide
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/48—Preparations in capsules, e.g. of gelatin, of chocolate
- A61K9/50—Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals
- A61K9/5073—Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals having two or more different coatings optionally including drug-containing subcoatings
- A61K9/5078—Microcapsules having a gas, liquid or semi-solid filling; Solid microparticles or pellets surrounded by a distinct coating layer, e.g. coated microspheres, coated drug crystals having two or more different coatings optionally including drug-containing subcoatings with drug-free core
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P25/00—Drugs for disorders of the nervous system
- A61P25/24—Antidepressants
Landscapes
- Health & Medical Sciences (AREA)
- Chemical & Material Sciences (AREA)
- Engineering & Computer Science (AREA)
- Organic Chemistry (AREA)
- Bioinformatics & Cheminformatics (AREA)
- Life Sciences & Earth Sciences (AREA)
- Animal Behavior & Ethology (AREA)
- General Health & Medical Sciences (AREA)
- Public Health (AREA)
- Veterinary Medicine (AREA)
- Pharmacology & Pharmacy (AREA)
- Medicinal Chemistry (AREA)
- Epidemiology (AREA)
- Psychiatry (AREA)
- Pain & Pain Management (AREA)
- Biomedical Technology (AREA)
- Neurology (AREA)
- Neurosurgery (AREA)
- Chemical Kinetics & Catalysis (AREA)
- General Chemical & Material Sciences (AREA)
- Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
- Medicinal Preparation (AREA)
- Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
Abstract
The present invention relates to stable dosage forms of levomilnacipran and pharmaceutically acceptable salts thereof. Processes for the preparation of these dosage forms and methods of using these dosage forms are also described.
Description
STABLE DOSAGE FORMS
OF LEVOMILNACIPRAN
This application claims priority under 35 U.S.C. 119(e) to U.S. Provisional Application No. 61/294,898, filed on January 14, 2010, and under 35 U.S.C. 120 to U.S.
Patent Application No. 12/941,293, filed on November 8, 2010, which claims priority under 35 U.S.C. 119(e) to U.S. Provisional Application No. 61/258,652, filed on November 6, 2009. The entire contents of these applications are incorporated herein by reference in their entirety.
FIELD OF THE INVENTION
The present invention relates to stable dosage formulations of levomilnacipran or a pharmaceutically acceptable salt thereof. Processes for the preparation of these dosage forms and methods of using these dosage forms are also described.
BACKGROUND OF THE INVENTION
Levomilnacipran is the international nonproprietary name for (IS, 2R)-2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide. It is a highly potent selective norepinephrine (NE) and serotonin (5-HT) reuptake inhibitor with greater selectivity for NE reuptake inhibition than for 5-HT reuptake inhibition. In particular, levomilnacipran has an inhibitory selectivity ratio for NE:5-HT of approximately 1.5:1.
Accordingly, levomilnacipran is considered a norepinephrine-serotonin reuptake inhibitor (NSRI) that is pharmacologically distinct from serotonin-norepinephrine reuptake inhibitors (SNRI) having equal or higher inhibitory selectivity for 5-HT than for NE.
While formulations of levomilnacipran are generally discussed in the prior art, difficulties have been encountered in preparing stable dosage forms of levomilnacipran.
These difficulties have arisen, at least in part, due to the sensitivity of levomilnacipran to certain reaction conditions and its reactivity with certain commonly-used excipients.
Accordingly, there is an existing and continual need for improved formulations of levomilnacipran having improved purity and stability. In addition, the improved-stability formulations must achieve a desirable pharmacokinetic profile that is associated with a low incidence of undesirable adverse events (for example, nausea, vomiting and gastric bleeding) in patients.
Improved formulations of levomilnacipran have now been discovered which achieve a desirable release of levomilnacipran upon entering a use environment and which have surprisingly high stability. These improved formulations of levomilnacipran are described herein.
SUMMARY OF THE INVENTION
The present invention relates to novel dosage forms of levomilnacipran, as well as processes for preparing these dosage forms and methods for using the dosage forms.
In some embodiments, the present invention relates to a stable dosage form that comprises levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a stable dosage form that comprises, or consists essentially of, an active ingredient that comprises substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a stable dosage form that comprises, or consists essentially of, an active ingredient that comprises at least about 98% by weight (e.g., at least 98% by weight) of levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof, wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 6.0 0.2 degrees 20.
OF LEVOMILNACIPRAN
This application claims priority under 35 U.S.C. 119(e) to U.S. Provisional Application No. 61/294,898, filed on January 14, 2010, and under 35 U.S.C. 120 to U.S.
Patent Application No. 12/941,293, filed on November 8, 2010, which claims priority under 35 U.S.C. 119(e) to U.S. Provisional Application No. 61/258,652, filed on November 6, 2009. The entire contents of these applications are incorporated herein by reference in their entirety.
FIELD OF THE INVENTION
The present invention relates to stable dosage formulations of levomilnacipran or a pharmaceutically acceptable salt thereof. Processes for the preparation of these dosage forms and methods of using these dosage forms are also described.
BACKGROUND OF THE INVENTION
Levomilnacipran is the international nonproprietary name for (IS, 2R)-2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide. It is a highly potent selective norepinephrine (NE) and serotonin (5-HT) reuptake inhibitor with greater selectivity for NE reuptake inhibition than for 5-HT reuptake inhibition. In particular, levomilnacipran has an inhibitory selectivity ratio for NE:5-HT of approximately 1.5:1.
Accordingly, levomilnacipran is considered a norepinephrine-serotonin reuptake inhibitor (NSRI) that is pharmacologically distinct from serotonin-norepinephrine reuptake inhibitors (SNRI) having equal or higher inhibitory selectivity for 5-HT than for NE.
While formulations of levomilnacipran are generally discussed in the prior art, difficulties have been encountered in preparing stable dosage forms of levomilnacipran.
These difficulties have arisen, at least in part, due to the sensitivity of levomilnacipran to certain reaction conditions and its reactivity with certain commonly-used excipients.
Accordingly, there is an existing and continual need for improved formulations of levomilnacipran having improved purity and stability. In addition, the improved-stability formulations must achieve a desirable pharmacokinetic profile that is associated with a low incidence of undesirable adverse events (for example, nausea, vomiting and gastric bleeding) in patients.
Improved formulations of levomilnacipran have now been discovered which achieve a desirable release of levomilnacipran upon entering a use environment and which have surprisingly high stability. These improved formulations of levomilnacipran are described herein.
SUMMARY OF THE INVENTION
The present invention relates to novel dosage forms of levomilnacipran, as well as processes for preparing these dosage forms and methods for using the dosage forms.
In some embodiments, the present invention relates to a stable dosage form that comprises levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a stable dosage form that comprises, or consists essentially of, an active ingredient that comprises substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a stable dosage form that comprises, or consists essentially of, an active ingredient that comprises at least about 98% by weight (e.g., at least 98% by weight) of levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof, wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 6.0 0.2 degrees 20.
2 In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 6.0, 12.0 and 20.1 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 22.5 0.2 degrees 20.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof and about 0.001% to about 0.5% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof and about 0.001% to about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof, and about 4 wt.% to about 10 wt.% of a binder.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof; about 30 wt.% to about 45 wt.% of an inert substrate or filler; and about 4 wt.% to about 10 wt.% of a binder.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof; about 30 wt.% to about 45 wt.% of an inert substrate or filler; about 4 wt.% to about 10 wt.% of a binder; and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof and about 0.001% to about 0.5% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof and about 0.001% to about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof, and about 4 wt.% to about 10 wt.% of a binder.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof; about 30 wt.% to about 45 wt.% of an inert substrate or filler; and about 4 wt.% to about 10 wt.% of a binder.
In some embodiments, the stable dosage form comprises about 45 wt.% to about 60 wt.% an active ingredient comprising substantially pure levomilnacipran or a pharmaceutically acceptable salt thereof; about 30 wt.% to about 45 wt.% of an inert substrate or filler; about 4 wt.% to about 10 wt.% of a binder; and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
3 In some embodiments, the stable dosage form comprises about 50 wt.% to about 60 wt.% of levomilnacipran or a pharmaceutically acceptable salt thereof;
about 30 wt.%
to about 40 wt.% of an inert substrate or filler; about 4 wt.% to about 8 wt.%
of a binder;
and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
In some embodiments, the stable dosage form comprises about 40% to about 55%
by weight of levomilnacipran or pharmaceutically acceptable salt thereof, about 5% to about 15% by weight of a release controlling agent, about 25% to about 40% by weight of an inert substrate, about 3% to about 10% by weight of a binder, about 3%
to about 10% by weight of an anti-adherent, and about 0.1% to about 5% by weight of a plasticizer.
In some embodiments, the stable dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 16 hours following entry into a use environment.
In some embodiments, the present invention relates to a stable oral dosage form comprising an active ingredient that comprises between about 10 mg and about 200 mg of levomilnacipran, wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 0.2 degrees 20.
In some embodiments, the present invention relates to an oral dosage form comprising between about 10 mg and about 200 mg of levomilnacipran and about 0.0001% to about 0.5% by weight (e.g., about 0.0001% to about 0.2% by weight or even about 0.0001% to about 0.1% by weight) of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0]
hexane-2-one.
In some embodiments, the present invention relates to an oral dosage form comprising between about 10 mg and about 200 mg of levomilnacipran and about 0.0001% to about 0.5% by weight (e.g., about 0.0001% to about 0.2% by weight or even about 0.0001% to about 0.1% by weight) of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0]
about 30 wt.%
to about 40 wt.% of an inert substrate or filler; about 4 wt.% to about 8 wt.%
of a binder;
and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
In some embodiments, the stable dosage form comprises about 40% to about 55%
by weight of levomilnacipran or pharmaceutically acceptable salt thereof, about 5% to about 15% by weight of a release controlling agent, about 25% to about 40% by weight of an inert substrate, about 3% to about 10% by weight of a binder, about 3%
to about 10% by weight of an anti-adherent, and about 0.1% to about 5% by weight of a plasticizer.
In some embodiments, the stable dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 16 hours following entry into a use environment.
In some embodiments, the present invention relates to a stable oral dosage form comprising an active ingredient that comprises between about 10 mg and about 200 mg of levomilnacipran, wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 0.2 degrees 20.
In some embodiments, the present invention relates to an oral dosage form comprising between about 10 mg and about 200 mg of levomilnacipran and about 0.0001% to about 0.5% by weight (e.g., about 0.0001% to about 0.2% by weight or even about 0.0001% to about 0.1% by weight) of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0]
hexane-2-one.
In some embodiments, the present invention relates to an oral dosage form comprising between about 10 mg and about 200 mg of levomilnacipran and about 0.0001% to about 0.5% by weight (e.g., about 0.0001% to about 0.2% by weight or even about 0.0001% to about 0.1% by weight) of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0]
4 hexane-2-one, wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 0.2 degrees 20.
In some embodiments, the dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 16 hours following entry into a use environment.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof and a release controlling agent, the dosage form sustaining release of the levomilnacipran or pharmaceutically acceptable salt thereof following entry of the dosage form into a use environment.
In some embodiments, the present invention relates to a stable oral dosage form comprising about 20 mg, about 40 mg, about 80mg or about 120 mg of levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a method for treating major depressive disorder comprising administering the stable dosage form of levomilnacipran or a pharmaceutically acceptable salt thereof to a patient in need thereof.
In some embodiments, the present invention relates to a method for treating major depressive disorder with concomitant fatigue comprising administering the stable dosage form of levomilnacipran or a pharmaceutically acceptable salt thereof to a patient in need thereof.
In some embodiments, the present invention relates to a method for preparing the stable dosage form, wherein the method comprises contacting an inert substrate with levomilnacipran or a pharmaceutically acceptable salt thereof and a dehydrated alcohol.
BRIEF DESCRIPTION OF THE FIGURES
Figure 1 shows the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention.
In some embodiments, the dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 16 hours following entry into a use environment.
In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof and a release controlling agent, the dosage form sustaining release of the levomilnacipran or pharmaceutically acceptable salt thereof following entry of the dosage form into a use environment.
In some embodiments, the present invention relates to a stable oral dosage form comprising about 20 mg, about 40 mg, about 80mg or about 120 mg of levomilnacipran or a pharmaceutically acceptable salt thereof.
In some embodiments, the present invention relates to a method for treating major depressive disorder comprising administering the stable dosage form of levomilnacipran or a pharmaceutically acceptable salt thereof to a patient in need thereof.
In some embodiments, the present invention relates to a method for treating major depressive disorder with concomitant fatigue comprising administering the stable dosage form of levomilnacipran or a pharmaceutically acceptable salt thereof to a patient in need thereof.
In some embodiments, the present invention relates to a method for preparing the stable dosage form, wherein the method comprises contacting an inert substrate with levomilnacipran or a pharmaceutically acceptable salt thereof and a dehydrated alcohol.
BRIEF DESCRIPTION OF THE FIGURES
Figure 1 shows the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention.
5 Figure 2 show the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention following one month of storage at 40 C and 75% relative humidity (RH).
Figure 3 show the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention following two months of storage at 40 C and 75% RH.
Figure 4 show the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention following three months of storage at 40 C and 75% RH.
Figure 5 show the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention following three months of storage at 40 C and 75% RH wherein the dosage form contained 1 gram of desiccant.
Figure 6 shows an X-ray powder diffraction pattern (XRD) for an active pharmaceutical ingredient comprising substantially pure levomilnacipran.
Figure 7 shows an XRD of a stable immediate-release dosage form of levomilnacipran in accordance with an embodiment of the invention.
Figure 8 shows an XRD of a stable sustained-release dosage form of levomilnacipran in accordance with an embodiment of the invention.
Figure 9 shows the mean plasma concentration of levomilnacipran versus time that may be achieved via single administration of Stable dosage forms of levomilnacipran to human patients.
DETAILED DESCRIPTION OF THE INVENTION
Novel stable dosage forms of levomilnacipran, methods of treatment using these dosage forms, and methods for preparing these dosage forms are provided herein. The dosage forms of levomilnacipran have been found to achieve a desirable dissolution profile upon entering a use environment and to have surprisingly high stability.
Figure 3 show the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention following two months of storage at 40 C and 75% RH.
Figure 4 show the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention following three months of storage at 40 C and 75% RH.
Figure 5 show the dissolution rates for a stable dosage form of levomilnacipran in accordance with an embodiment of the present invention following three months of storage at 40 C and 75% RH wherein the dosage form contained 1 gram of desiccant.
Figure 6 shows an X-ray powder diffraction pattern (XRD) for an active pharmaceutical ingredient comprising substantially pure levomilnacipran.
Figure 7 shows an XRD of a stable immediate-release dosage form of levomilnacipran in accordance with an embodiment of the invention.
Figure 8 shows an XRD of a stable sustained-release dosage form of levomilnacipran in accordance with an embodiment of the invention.
Figure 9 shows the mean plasma concentration of levomilnacipran versus time that may be achieved via single administration of Stable dosage forms of levomilnacipran to human patients.
DETAILED DESCRIPTION OF THE INVENTION
Novel stable dosage forms of levomilnacipran, methods of treatment using these dosage forms, and methods for preparing these dosage forms are provided herein. The dosage forms of levomilnacipran have been found to achieve a desirable dissolution profile upon entering a use environment and to have surprisingly high stability.
6 Definitions As used herein, the term "levomilnacipran" refers to (1 S,2R)-2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide and pharmaceutically acceptable salts thereof. The term is not inclusive of other isomers of 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide (e.g., 1R,2S 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide) or degradants of (1S,2R)-2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide (e.g., (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0]
hexane-2-one). The term "pharmaceutically acceptable salt" refers to any salt of levomilnacipran that is physiologically tolerated by a patient (for example, levomilnacipran hydrochloride). The structural formula of levomilnacipran is shown below:
NH~
(1) The term "substantially pure levomilnacipran" is used herein to mean at least 98%
by weight of levomilnacipran. For example, an active pharmaceutical ingredient (i.e., active ingredient) that comprises substantially pure levomilnacipran comprises at least 98% by weight (e.g., about 98.5% by weight) of levomilnacipran and at most 2%
by weight of total combined other components (such as other isomers of 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide and/or degradants of (1S,2R)-2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide).
The term "stable", when used herein to refer to the dosage form means that the dosage form comprises an active ingredient that comprises substantially pure levomilnacipran.
The terms "dehydrated alcohol" and "dehydrated solvent" are defined herein as they are defined in the U.S. Pharmacopeia to mean an alcohol or solvent that contains less than or equal to 0.8% by weight of water, which corresponds to less or equal to
hexane-2-one). The term "pharmaceutically acceptable salt" refers to any salt of levomilnacipran that is physiologically tolerated by a patient (for example, levomilnacipran hydrochloride). The structural formula of levomilnacipran is shown below:
NH~
(1) The term "substantially pure levomilnacipran" is used herein to mean at least 98%
by weight of levomilnacipran. For example, an active pharmaceutical ingredient (i.e., active ingredient) that comprises substantially pure levomilnacipran comprises at least 98% by weight (e.g., about 98.5% by weight) of levomilnacipran and at most 2%
by weight of total combined other components (such as other isomers of 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide and/or degradants of (1S,2R)-2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide).
The term "stable", when used herein to refer to the dosage form means that the dosage form comprises an active ingredient that comprises substantially pure levomilnacipran.
The terms "dehydrated alcohol" and "dehydrated solvent" are defined herein as they are defined in the U.S. Pharmacopeia to mean an alcohol or solvent that contains less than or equal to 0.8% by weight of water, which corresponds to less or equal to
7 99.5% by volume of water. The term "dehydrated solvent" is used herein synonymously with the terms "substantially pure solvent," "anhydrous solvent," and "absolute solvent".
Likewise, the term "dehydrated alcohol" is used herein synonymously with the terms "substantially pure alcohol," "anhydrous alcohol," and "absolute alcohol".
The term "treating" is used herein, unless otherwise indicated, to mean to relieve, alleviate, delay, reduce, reverse, improve or prevent at least one symptom of a disease, disorder or condition in a patient which may be treated by inhibition of norepinephrine (NE) and serotonin (5-HT) reuptake. The term "treating" may also mean to arrest, delay the onset (i.e., the period prior to clinical manifestation of a disease, disorder or condition) and/or reduce the risk of developing or worsening a disease, disease or condition which may be treated by inhibition of norepinephrine (NE) and serotonin (5-HT) reuptake.
The terms "dosage form" is used herein, unless otherwise indicated, to refer to any formulation of levomilnacipran that is suitable for oral administration to a human patient. For example, the term "dosage form" encompasses any oral dosage form or any solid oral dosage form, for example, compositions that are suitable for loading into capsules (e.g., beads, granules, microgranules, or the like), tablets, gelcaps, caplets, lozenges or powders). In some embodiments, the dosage form is a dosage form (e.g., bead, granule, microgranule or the like) that is suited for loading into capsules. In some embodiments, the dosage form is an immediate-release dosage form (e.g., an immediate-release solid dosage form, an immediate-release oral dosage form or an immediate-release solid oral dosage form).
In some embodiments, the dosage form is an immediate-release composition that is coated with a modified-release (e.g., sustained-release, delayed-release and/or extended release) composition. In some embodiments, the dosage form is a sustained-release dosage form (e.g., a sustained-release solid dosage form, a sustained-release oral dosage form, or a sustained-release solid oral dosage form). In some embodiments, the dosage form is a capsule (e.g., a bead-, granule- or microgranule-filled capsule). In some embodiments, the dosage form is a tablet. In some embodiments, the dosage form is a
Likewise, the term "dehydrated alcohol" is used herein synonymously with the terms "substantially pure alcohol," "anhydrous alcohol," and "absolute alcohol".
The term "treating" is used herein, unless otherwise indicated, to mean to relieve, alleviate, delay, reduce, reverse, improve or prevent at least one symptom of a disease, disorder or condition in a patient which may be treated by inhibition of norepinephrine (NE) and serotonin (5-HT) reuptake. The term "treating" may also mean to arrest, delay the onset (i.e., the period prior to clinical manifestation of a disease, disorder or condition) and/or reduce the risk of developing or worsening a disease, disease or condition which may be treated by inhibition of norepinephrine (NE) and serotonin (5-HT) reuptake.
The terms "dosage form" is used herein, unless otherwise indicated, to refer to any formulation of levomilnacipran that is suitable for oral administration to a human patient. For example, the term "dosage form" encompasses any oral dosage form or any solid oral dosage form, for example, compositions that are suitable for loading into capsules (e.g., beads, granules, microgranules, or the like), tablets, gelcaps, caplets, lozenges or powders). In some embodiments, the dosage form is a dosage form (e.g., bead, granule, microgranule or the like) that is suited for loading into capsules. In some embodiments, the dosage form is an immediate-release dosage form (e.g., an immediate-release solid dosage form, an immediate-release oral dosage form or an immediate-release solid oral dosage form).
In some embodiments, the dosage form is an immediate-release composition that is coated with a modified-release (e.g., sustained-release, delayed-release and/or extended release) composition. In some embodiments, the dosage form is a sustained-release dosage form (e.g., a sustained-release solid dosage form, a sustained-release oral dosage form, or a sustained-release solid oral dosage form). In some embodiments, the dosage form is a capsule (e.g., a bead-, granule- or microgranule-filled capsule). In some embodiments, the dosage form is a tablet. In some embodiments, the dosage form is a
8 once-daily solid oral dosage form. In some embodiments, the dosage form is a once-daily capsule.
The term "sustained release" is used herein, unless otherwise indicated, to refer to dosage forms that release levomilnacipran (and optionally additional active agents contained therein) at a time other than promptly after administration, e.g., over an extended period of time that exceeds the duration of drug release from conventional instant- and immediate-release dosage forms of levomilnacipran.
The term "entry into a use environment" is used herein, unless otherwise indicated, to refer to contact of the stable dosage form of levomilnacipran with gastric or intestinal fluid of a patient to whom it is administered, with a fluid intended to simulate gastric or intestinal fluid, or with deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm (for example, with 1000 mL of deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm).
As used herein, unless otherwise indicated, dissolution rates define the percentage of levomilnacipran originally contained in an stable dosage form that is released from the dosage form within a specified period of time following entry of the dosage form into a use environment.
As used herein, unless otherwise indicated, the terms "effective amount" and "therapeutically effective amount" refer to an amount or quantity of levomilnacipran which is sufficient to elicit an appreciable biological response when administered to a patient. For example, the terms "effective amount" and "therapeutically effective amount" refer to an amount of levomilnacipran (or additional active agent contained in the dosage form) that, when administered to a patient (e.g., human or other mammal) for treating a disease, condition or disorder which may be treated by inhibition of norepinephrine (NE) and serotonin (5-HT) reuptake (e.g., major depressive disorder or anxiety), is sufficient to effect such treatment of one or more symptoms of the disease, disorder or condition, or an amount of levomilnacipran (or additional active agent contained in the dosage form) that is sufficient for inhibition of NE and 5-HT
reuptake in a patient. It will be appreciated that the precise therapeutic dose will depend on the age,
The term "sustained release" is used herein, unless otherwise indicated, to refer to dosage forms that release levomilnacipran (and optionally additional active agents contained therein) at a time other than promptly after administration, e.g., over an extended period of time that exceeds the duration of drug release from conventional instant- and immediate-release dosage forms of levomilnacipran.
The term "entry into a use environment" is used herein, unless otherwise indicated, to refer to contact of the stable dosage form of levomilnacipran with gastric or intestinal fluid of a patient to whom it is administered, with a fluid intended to simulate gastric or intestinal fluid, or with deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm (for example, with 1000 mL of deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm).
As used herein, unless otherwise indicated, dissolution rates define the percentage of levomilnacipran originally contained in an stable dosage form that is released from the dosage form within a specified period of time following entry of the dosage form into a use environment.
As used herein, unless otherwise indicated, the terms "effective amount" and "therapeutically effective amount" refer to an amount or quantity of levomilnacipran which is sufficient to elicit an appreciable biological response when administered to a patient. For example, the terms "effective amount" and "therapeutically effective amount" refer to an amount of levomilnacipran (or additional active agent contained in the dosage form) that, when administered to a patient (e.g., human or other mammal) for treating a disease, condition or disorder which may be treated by inhibition of norepinephrine (NE) and serotonin (5-HT) reuptake (e.g., major depressive disorder or anxiety), is sufficient to effect such treatment of one or more symptoms of the disease, disorder or condition, or an amount of levomilnacipran (or additional active agent contained in the dosage form) that is sufficient for inhibition of NE and 5-HT
reuptake in a patient. It will be appreciated that the precise therapeutic dose will depend on the age,
9 condition, weight, etc. of the patient and the nature of the condition being treated and will be ultimately be at the discretion of the attending physician.
For example, in some embodiments, the therapeutically effective dosage of levomilnacipran within the stable dosage form for treating depression (e.g., major depressive disorder) was found to be between about 10mg and about 150mg of an active ingredient comprising substantially pure levomilnacipran (e.g., between about 20mg and about 120mg of the active ingredient). In some embodiments, the dosage form comprises between about 15mg and about 25mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 20mg). In some embodiments, the dosage form comprises between about 35mg and about 45mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 40mg). In some embodiments, the dosage form comprises between about 70 mg and about 90 mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 80mg). In some embodiments, the dosage form comprises between about 100mg and about 140mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 120mg).
As used herein, unless otherwise indicated, the term "purity" when used in referring to the stable dosage forms means the degree to which the dosage form is free from (or lacks) specific undesirable components or impurities (for example, degradants or the like).
The term "consisting essentially of', when used in reference to the dosage form, means that the dosage form contains no additional active pharmaceutical ingredients but may contain additional inactive components or excipients.
As used herein, unless otherwise indicated, the terms "about" and "approximately" should be understood to mean within an acceptable error range for the particular value as determined by one of ordinary skill in the art, which will depend in part on how the value is measured or determined, i.e., the limitations of the measurement system. For example, "about" can mean within 1 or more than 1 standard deviations, per the practice in the art. Alternatively, "about" can mean a range of up to 20%, preferably up to 10%, more preferably up to 5%, and more preferably still up to 1 % of a given value.
X-Ray Powder Diffraction Pattern of Oral Dosage Form In some preferred embodiments, the stable dosage form, or the active ingredient contained within the dosage form, is crystalline in structure. In some preferred embodiments, the stable dosage form and the active ingredient contained within the dosage form are crystalline in structure. In some embodiments, the stable dosage form has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 1. In some embodiments, the stable dosage form comprises an active ingredient comprising levomilnacipran wherein the active ingredient has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 1.
As used herein, unless otherwise indicated, the phrase "one or more peaks"
should be understood to be inclusive of (i) stable dosage forms that have XRD peaks at every peak value recited after this phrase, (ii) stable dosage forms that have an XRD peak at only one of the peak values recited after this phrase, as well (iii) stable dosage forms that have XRD peaks at two or more (e.g., three or more, four or more, five or more, six or more, or even seven or more) of the peak values recited after this phrase.
Table 1 2-Theta d(,A) 2-Theta d(A) 6.0 14.8 22.4 4.0 12.0 7.4 24.1 3.7 12.4 7.1 24.6 3.6 14.2 6.2 24.8 3.6 17.4 5.1 28.8 3.1 18.2 4.9 30.7 2.9 20.1 4.4 32.7 2.7 21.1 4.2 35.2 2.5 21.6 4.1 In some embodiments, the stable dosage form of levomilnacipran has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 2.
Table 2 2-Theta d(,k) 2-Theta d(A) 2.3 39.2 20.0 4.4 5.9 14.9 21.7 4.1 9.5 9.3 22.4 4.0 11.9 7.4 24.5 3.6 12.3 7.2 28.6 3.1 14.1 6.3 30.6 2.9 16.5 5.4 32.7 2.7 17.3 5.1 34.5 2.6 18.1 4.9 In some embodiments, the stable dosage form of levomilnacipran is a modified-release dosage form (e.g., a sustain-release dosage form) and has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 3.
Table 3 2-Theta d(A) 2-Theta (1(,A) 6.0 14.7 22.1 4.0 8.3 10.6 22.5 4.0 9.6 9.2 23.6 3.8 12.0 7.4 24.7 3.6 12.8 6.9 25.2 3.5 13.1 6.7 26.4 3.4 14.2 6.2 27.5 3.2 15.6 5.7 28.7 3.1 16.4 5.4 30.6 2.9 16.8 5.3 31.0 2.9 17.4 5.1 32.0 2.8 18.3 4.8 32.7 2.7 18.9 4.7 33.5 2.7 19.6 4.5 34.6 2.6 20.0 4.4 36.2 2.5 20.4 4.4 37.3 2.4 20.9 4.2 38.3 2.3 21.6 4.1 In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 6.0 0.2 degrees 20.
In some embodiments, the stable dosage form of levomilnacipran has an XRD
comprising characteristic peaks at about 6.0, about 12.0 and about 20.1 0.2 degrees 20.
In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0, about 12.0 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0, about 12.0, about 20.1 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0, about 20.1 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD
comprising characteristic peaks at about 12.0, about 20.1 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0 and about 12.0 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0 and about 20.1 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD
comprising characteristic peaks at about 6.0 and about 22.4 0.2 degrees 20.
In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 12.0 and about 20.1 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 12.0 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 20.1 0.2 degrees 20 and at about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form comprises a crystalline form of levomilnacipran having an XRD that comprises characteristic peaks at one or more of about 6.0 0.2 degrees 20, about 12.0 0.2 degrees 20, about 20.1 0.2 degrees 20 and about 22.4 0.2 degrees 20.
In some embodiments, the stable dosage form comprises an active ingredient that comprises substantially pure levomilnacipran wherein the active ingredient comprises one or more of the characteristic peaks shown in Table 1. In some embodiments, the stable dosage form comprises an active ingredient that comprises substantially pure levomilnacipran wherein the stable dosage form comprises one or more of the characteristic peaks shown in Table 1 or Table 2.
Purity of the Stable Dosage Forms The stable dosage form and the active ingredient in the dosage form have been found to comprise a surprisingly low concentration of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, which is represented by Formula (II):
llllnnõ
O N
N (II).
In some embodiments, the stable dosage form comprises about 0.0001 to about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, as defined by the International Conference on Harmonization (ICH) guidelines, for example after storage for one, two or three months of storage at 40 C and 75% relative humidity. In some embodiments, the stable dosage form comprises less than about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, for example after storage for one, two or three months of storage at 40 C and 75% relative humidity. In some embodiments, the stable dosage form comprises about 0.0001 to about 0.1% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, for example, after storage for one, two or three months of storage at 40 C and 75% relative humidity.
In some preferred embodiments, the stable dosage form comprises about 0.001 to about 0.2 wt.%, about 0.01 to about 0.2 wt.%, about 0.0001 to about 0.15 wt.%, about 0.001 to about 0.15 wt.%, about 0.01 to about 0.15 wt.%, about 0.001 to about 0.1 wt.%, about 0.01 to about 0.1 wt.%, about 0.01 to about 0.08 wt.%, or even about 0.001 to about 0.08 wt.% of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, for example, after storage for one, two, three, four, five or six months of storage at 40 C
and 75%
relative humidity. In some embodiments, the stable dosage form comprises about 0.01 to about 0.08 wt.% (e.g., about 0.001 to about 0.08 wt.%) of (1S, 5R) 1-phenyl-3-azabicyclo [3 - 1 -0] hexane-2-one, for example, after storage for one, two, three, four, five or six months of storage at 40 C and 75% relative humidity.
Preparation of the Stable Dosage Form The stable dosage forms of levomilnacipran can be prepared by any suitable process. In some preferred embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution that comprises (or consists essentially of or consists of) levomilnacipran, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) (e.g., a dehydrated alcohol such as 200-proof ethanol) and optionally a binder and an anti-adherent or lubricant, to form a levomilnacipran composition. In some embodiments, the dosage forms of levomilnacipran are then coated to render them sustained-release dosage forms by contacting the levomilnacipran composition with a solution that comprises a release controlling agent, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) (e.g., a dehydrated alcohol such as 200-proof ethanol) and optionally a plasticizer, an anti-adherent or glidant.
In some preferred embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution that comprises levomilnacipran, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water), a binder, and an anti-adherent or lubricant, to form a levomilnacipran composition. In some embodiments, the dosage forms of levomilnacipran are then coated to render them sustained-release dosage forms by contacting the levomilnacipran composition with a solution that comprises a release controlling agent, a plasticizer, an anti-adherent or glidant, and a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with levomilnacipran and optionally a binder, an anti-adherent or lubricant, and/or a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) to form a levomilnacipran composition (e.g., a levomilnacipran core or levomilnacipran beads or granules). In some embodiments, the dosage forms of levomilnacipran are then coated to render them sustained-release dosage forms by contacting the levomilnacipran composition with a release controlling agent and optionally a plasticizer, an anti-adherent or lubricant; and/or a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution that comprises levomilnacipran, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) and optionally a binder and an anti-adherent (or lubricant) to form a levomilnacipran composition (e.g., a core, bead or granule comprising levomilnacipran). In some embodiments, the method further comprises coating the levomilnacipran composition with a solution that comprises (or consists essentially of or consists of) a release controlling agent and optionally a plasticizer, an anti-adherent or lubricant; and/or a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution comprising levomilnacipran, a binder, an anti-adherent or lubricant, and a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the contacting step comprises layering the inert substrate with a drug layering solution that consists essentially of levomilnacipran, a binder, an anti-adherent (or lubricant) and a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some preferred embodiments, the contacting step (e.g., drug layering step) is performed by a Wurster process (e.g., within a Wurster apparatus) or the like.
In some preferred embodiments, the coating step is performed by a Wurster process (e.g., within a Wurster apparatus) or the like. In some preferred embodiments, the combining step and the contacting steps are both performed by a Wurster process or the like.
The process for determining the relative percentages of levomilnacipran and other isomers of 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide (e.g., 1R,2S 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide) in the active pharmaceutical ingredient can be performed using any suitable method, preferably by reverse phase high performance liquid chromatograph (RP HPLC) (for example, with a UV detection at 220 nm).
Components of the stable dosage forms The stable dosage form can comprise any therapeutically effective amount of levomilnacipran. In some embodiments, the stable dosage form comprises about 5 to about 200 mg of levomilnacipran. In some embodiments, the stable dosage form comprises about 10 to about 180 mg of levomilnacipran. In some embodiments, the stable dosage form comprises about 20 to about 150 mg of levomilnacipran. In some embodiments, the stable dosage form comprises about 20 to about 120 mg of levomilnacipran. For example, the stable dosage form can comprise about 20 mg, about 40 mg, about 50 mg, about 60 mg, about 80 mg, about 100 mg, 120 mg, or about 240 mg of levomilnacipran. In this regard, the stable dosage form can comprise any suitable weight percentage of levomilnacipran relative to other components of the dosage form.
For example, the stable dosage form can comprise about 35 to about 65% by weight (e.g., about 35 to about 60 wt.%, about 35 to about 55 wt.%, about 40 to about 55 wt.%, or about 40 to about 50 wt.%) of levomilnacipran.
The stable dosage form of levomilnacipran also comprises an inert substrate or filler. In some preferred embodiments, the stable dosage form comprises an inert substrate that comprises sugar for example sucrose (e.g., sugar spheres).
Other suitable inert substrates or fillers include, for example, isomalt, dicalcium phosphate dihydrate, calcium sulfate, lactose, mannitol, sorbitol, cellulose, microcrystalline cellulose, kaolin, sodium chloride, dry starch, hydrolyzed starches, pre-gelatinized starch, silicone dioxide, titanium oxide, magnesium aluminum silicate, or a mixture thereof.
The stable dosage form can comprise any suitable amount of the inert substrate or filler (e.g., sugar spheres). In some embodiments, the stable dosage form comprises about 15 to about 45% by weight of the inert substrate or filler. In some embodiments, the stable dosage form comprises about 20 to about 40 wt.% of the inert substrate or filler. In some embodiments, the stable dosage form comprises about 25 to about 40 wt.% of the inert substrate or filler. In some embodiments, the stable dosage form comprises about 30 to about 40 wt.% of the inert substrate or filler In some embodiments, the stable dosage form comprises about 35 to about 40 wt.% of the inert substrate or filler.
The stable dosage form can comprise sugar spheres in any suitable size. In some embodiments, the stable dosage form comprises sugar spheres having a size of about 20 to about 50 mesh. In some embodiments, the stable dosage form comprises sugar spheres having a size of approximately about 25 to about 45 mesh. In some embodiments, the stable dosage form comprises sugar spheres having a size of about 25 to about 40 mesh.
In some preferred embodiments, the stable dosage form comprises sugar spheres having a size of approximately about 30 to about 40 mesh (for example, about 30 to about 35 mesh). For example, the stable dosage form may comprise about 30 to about 40 wt.%
(e.g., about 35 to about 40 wt.%) of sugar spheres having a size of about 30 to about 40 mesh.
The stable dosage form also comprises a binder in some preferred embodiments, for example polyvinyl pyrrolidone (e.g., Povidone K30). Other suitable binders include, for example, starch, polyvinyl alcohol, pre-gelatinized starch, gelatin, sucrose, glucose, dextrose, lactose, sorbitol, polyethylene glycol, waxes, natural and synthetic gums such as acacia, tragacanth, sodium alginate, hydroxypropylmethylcellulose, hydroxypropylcellulose, ethylcellulose, veegum, and synthetic polymers such as acrylic acid and methacrylic acid copolymers, methacrylic acid copolymers, methyl methacrylate copolymers, aminoalkyl methacrylate copolymers, polyacrylic acid/polymethacrylic acid, or a mixture thereof.
The stable dosage form can comprise any suitable amount of the binder (e.g., PVP). In some embodiments, the stable dosage form comprises about 0.1 to about 15%
by weight of a binder. In some embodiments, the stable dosage form comprises about 1 to about 12% by weight of a binder. In some embodiments, the stable dosage form comprises about 1 to about 10% by weight of a binder. In some embodiments, the stable dosage form comprises about 2 to about 10% by weight of a binder.
In some preferred embodiments, the stable dosage form comprises about 3 to about 10% by weight of a binder (e.g., PVP). In some embodiments, the stable dosage form comprises about 4 to about 10% by weight of the binder. In some embodiments, the stable dosage form comprises about 2 to about 8% by weight of the binder. In some embodiments, the stable dosage form comprises about 4 to about 8% by weight of the binder. In some embodiments, the stable dosage form comprises about 5 to about 7% by weight of the binder.
The stable dosage form also comprises an anti-adherent or lubricant in some preferred embodiments, for example, talc. Other suitable anti-adherents or lubricants include, for example, magnesium stearate, calcium stearate, stearic acid, glycerol behenate, polyethylene glycol, talc, mineral oil, sodium stearyl fumarate or mixtures thereof.
The stable dosage form can comprise any suitable amount of the lubricant or anti-adherent (for example, talc). In some embodiments, the stable dosage form comprises about 0.1 to about 15% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 1 to about 12% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 2 to about 10% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 3 to about 10% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 4 to about 10%
by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 4 to about 8% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 5 to about 8% by weight of the lubricant or anti-adherent.
In some preferred embodiments, the stable dosage form comprises about 4 to about 7.5% by weight of the lubricant or anti-adherent. In some preferred embodiments, the stable dosage form comprises about 5 to about 7% by weight of the lubricant or anti-adherent.
In some embodiments, the stable dosage form is a sustained-release (SR) dosage form and comprises a release controlling agent, polymeric agent or coating polymer (e.g., ethyl cellulose) which substantially contributes to sustaining the release of levomilnacipran from the dosage form. Other suitable release controlling agents include, for example, a cellulose and cellulose derivative, wax, carbomer, polyalkylene polyol, polycarbophil, methacrylic acid derivative, gelatin, gum, polyethylene oxide, and polyvinyl pyrrolidone, or mixtures thereof. In some embodiments, the release controlling agent, polymeric additive or coating polymer is selected from ethyl cellulose, hydroxypropyl cellulose, hydroxyethyl cellulose, hydroxymethyl cellulose, hydroxypropyl methyl cellulose, hydroxypropyl methyl cellulose acetate succinate, hydroxypropylmethyl cellulose phthalate, methylcellulose, cellulose acetate, cellulose acetate phthalate, cellulose acetate trimellitate and carboxymethylcellulose sodium;
acrylic acid polymers and copolymers (preferably formed from acrylic acid, methacrylic acid, methyl acrylate, ethyl acrylate, methyl methacrylate and/or ethyl methacrylate), and other methacrylic resins that are commercially available under the trade name EudragitTM
(Rohm Pharma; Westerstadt, Germany), including EudragitTM L30D-55 and L100-55, EudragitTM, EudragitTM and EudragitTM NE, RL and RS; vinyl polymers and copolymers such as polyvinyl pyrrolidone, vinyl acetate, vinyl acetate phthalate, vinyl acetate crotonic acid copolymer, and ethylene-vinyl acetate copolymer; enzymatically degradable polymers such as azo polymers, pectin, chitosan, amylose and guar gum; zein and shellac, or mixtures thereof.
The stable dosage form can comprise any suitable amount of the release controlling agent, polymeric agent or coating polymer (e.g., ethyl cellulose).
The stable dosage form preferably comprises about 5 to about 15% by weight of the release controlling agent, polymeric agent or coating polymer. However, n some embodiments, the stable dosage form comprises about 2 to about 20% by weight of a release controlling agent, polymeric agent or coating polymer. In some embodiments, the stable dosage form comprises about 5 to about 12% by weight of a release controlling agent, polymeric agent or coating polymer. In some embodiments, the stable dosage form comprises about 8 to about 12% by weight of a release controlling agent, polymeric agent or coating polymer. In some embodiments, the stable dosage form comprises about 8 to about 11%
by weight of a release controlling agent, polymeric agent or coating polymer.
In some embodiments, the stable dosage form comprises about 8 to about 10% by weight of a release controlling agent, polymeric agent or coating polymer.
The stable dosage form also comprises a plasticizer in some preferred embodiments, for example triethyl citrate. Other suitable plasticizers include, for example, polyethylene glycol, propylene glycol, triacetin, dimethyl phthalate, diethyl phthalate, dibutyl phthalate, dibutyl sebacate, tributyl citrate, triethyl acetyl citrate, glycerol monostearate, castor oil, acetylated monoglycerides, or a mixture thereof.
The stable dosage form can comprise any suitable amount of the plasticizer (for example, triethyl citrate). In some embodiments, the stable dosage form comprises about 0.1 to about 10% by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 0.5 to about 8% by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 0.5 to about 5% by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 1 to about 5%
by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 1 to about 3% by weight of the plasticizer.
In addition, the stable dosage form of levomilnacipran can comprise any additional excipients or additives in some embodiments, such as plasticizers, pigments, colorants, stabilizing agents, glidants, or the like.
In some preferred embodiments, the dosage form comprises about 30 wt.% to about 65 wt.% (e.g., about 40 wt.% to about 60 wt.%, about 45 wt.% to about 60 wt.% or even about 50 wt.% to about 60 wt.%) of levomilnacipran (or an active ingredient comprising at least 98% by weight or even substantially pure levomilnacipran);
about 25 wt.% to about 55 wt.% (e.g., about 30 wt.% to about 45 wt.% or even about 30 wt.% to about 40 wt.%) of an inert substrate or filler; about 2 wt.% to about 12 wt.%
(e.g., about 4 wt.% to about 10 wt.% or even about 4 wt.% to about 8 wt.%) of a binder; and about 0.5 wt.% to about 10 wt.% (e.g., about 1 wt.% to about 8 wt.%, about 1 wt.% to about 5 wt.%
or even about 2 wt.% to about 5 wt.%) of an anti-adherent or lubricant.
In some preferred embodiments, the dosage form comprises about 45 wt.% to about 60 wt.% of levomilnacipran (or an active ingredient comprising at least 98% by weight or even substantially pure levomilnacipran); about 30 wt.% to about 45 wt.% of an inert substrate or filler; about 4 wt.% to about 10 wt.% of a binder; and about 1 wt.%
to about 5 wt.% of an anti-adherent or lubricant.
In some preferred embodiments, the dosage form comprises about 50 wt.% to about 60 wt.% of levomilnacipran (or an active ingredient comprising at least 98% by weight or even substantially pure levomilnacipran); about 30 wt.% to about 40 wt.% of an inert substrate or filler; about 4 wt.% to about 8 wt.% of a binder; and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); and about 0.1 to about 4 wt.%
(e.g., about 1 to about 3 wt.%) of a plasticizer (e.g., triethyl citrate).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
and about 0.1 to about 4 wt.% (e.g., about 1 to about 3 wt.%) of a plasticizer (e.g., triethyl citrate).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
and about 0.1 to about 4 wt.% (e.g., about 1 to about 3 wt.%) of a plasticizer (e.g., triethyl citrate).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); and about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
and about 5-
For example, in some embodiments, the therapeutically effective dosage of levomilnacipran within the stable dosage form for treating depression (e.g., major depressive disorder) was found to be between about 10mg and about 150mg of an active ingredient comprising substantially pure levomilnacipran (e.g., between about 20mg and about 120mg of the active ingredient). In some embodiments, the dosage form comprises between about 15mg and about 25mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 20mg). In some embodiments, the dosage form comprises between about 35mg and about 45mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 40mg). In some embodiments, the dosage form comprises between about 70 mg and about 90 mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 80mg). In some embodiments, the dosage form comprises between about 100mg and about 140mg of an active ingredient comprising substantially pure levomilnacipran (e.g., about 120mg).
As used herein, unless otherwise indicated, the term "purity" when used in referring to the stable dosage forms means the degree to which the dosage form is free from (or lacks) specific undesirable components or impurities (for example, degradants or the like).
The term "consisting essentially of', when used in reference to the dosage form, means that the dosage form contains no additional active pharmaceutical ingredients but may contain additional inactive components or excipients.
As used herein, unless otherwise indicated, the terms "about" and "approximately" should be understood to mean within an acceptable error range for the particular value as determined by one of ordinary skill in the art, which will depend in part on how the value is measured or determined, i.e., the limitations of the measurement system. For example, "about" can mean within 1 or more than 1 standard deviations, per the practice in the art. Alternatively, "about" can mean a range of up to 20%, preferably up to 10%, more preferably up to 5%, and more preferably still up to 1 % of a given value.
X-Ray Powder Diffraction Pattern of Oral Dosage Form In some preferred embodiments, the stable dosage form, or the active ingredient contained within the dosage form, is crystalline in structure. In some preferred embodiments, the stable dosage form and the active ingredient contained within the dosage form are crystalline in structure. In some embodiments, the stable dosage form has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 1. In some embodiments, the stable dosage form comprises an active ingredient comprising levomilnacipran wherein the active ingredient has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 1.
As used herein, unless otherwise indicated, the phrase "one or more peaks"
should be understood to be inclusive of (i) stable dosage forms that have XRD peaks at every peak value recited after this phrase, (ii) stable dosage forms that have an XRD peak at only one of the peak values recited after this phrase, as well (iii) stable dosage forms that have XRD peaks at two or more (e.g., three or more, four or more, five or more, six or more, or even seven or more) of the peak values recited after this phrase.
Table 1 2-Theta d(,A) 2-Theta d(A) 6.0 14.8 22.4 4.0 12.0 7.4 24.1 3.7 12.4 7.1 24.6 3.6 14.2 6.2 24.8 3.6 17.4 5.1 28.8 3.1 18.2 4.9 30.7 2.9 20.1 4.4 32.7 2.7 21.1 4.2 35.2 2.5 21.6 4.1 In some embodiments, the stable dosage form of levomilnacipran has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 2.
Table 2 2-Theta d(,k) 2-Theta d(A) 2.3 39.2 20.0 4.4 5.9 14.9 21.7 4.1 9.5 9.3 22.4 4.0 11.9 7.4 24.5 3.6 12.3 7.2 28.6 3.1 14.1 6.3 30.6 2.9 16.5 5.4 32.7 2.7 17.3 5.1 34.5 2.6 18.1 4.9 In some embodiments, the stable dosage form of levomilnacipran is a modified-release dosage form (e.g., a sustain-release dosage form) and has an X-ray powder diffraction pattern (XRD) comprising one or more characteristic peaks as provided in Table 3.
Table 3 2-Theta d(A) 2-Theta (1(,A) 6.0 14.7 22.1 4.0 8.3 10.6 22.5 4.0 9.6 9.2 23.6 3.8 12.0 7.4 24.7 3.6 12.8 6.9 25.2 3.5 13.1 6.7 26.4 3.4 14.2 6.2 27.5 3.2 15.6 5.7 28.7 3.1 16.4 5.4 30.6 2.9 16.8 5.3 31.0 2.9 17.4 5.1 32.0 2.8 18.3 4.8 32.7 2.7 18.9 4.7 33.5 2.7 19.6 4.5 34.6 2.6 20.0 4.4 36.2 2.5 20.4 4.4 37.3 2.4 20.9 4.2 38.3 2.3 21.6 4.1 In some embodiments, the present invention relates to a stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof wherein the dosage form comprises a X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 32.7 0.2 degrees 20. In some embodiments, the XRD pattern also comprises a characteristic peak at 6.0 0.2 degrees 20.
In some embodiments, the stable dosage form of levomilnacipran has an XRD
comprising characteristic peaks at about 6.0, about 12.0 and about 20.1 0.2 degrees 20.
In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0, about 12.0 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0, about 12.0, about 20.1 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0, about 20.1 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD
comprising characteristic peaks at about 12.0, about 20.1 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0 and about 12.0 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 6.0 and about 20.1 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD
comprising characteristic peaks at about 6.0 and about 22.4 0.2 degrees 20.
In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 12.0 and about 20.1 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 12.0 and about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form has an XRD comprising characteristic peaks at about 20.1 0.2 degrees 20 and at about 22.4 0.2 degrees 20. In some embodiments, the stable dosage form comprises a crystalline form of levomilnacipran having an XRD that comprises characteristic peaks at one or more of about 6.0 0.2 degrees 20, about 12.0 0.2 degrees 20, about 20.1 0.2 degrees 20 and about 22.4 0.2 degrees 20.
In some embodiments, the stable dosage form comprises an active ingredient that comprises substantially pure levomilnacipran wherein the active ingredient comprises one or more of the characteristic peaks shown in Table 1. In some embodiments, the stable dosage form comprises an active ingredient that comprises substantially pure levomilnacipran wherein the stable dosage form comprises one or more of the characteristic peaks shown in Table 1 or Table 2.
Purity of the Stable Dosage Forms The stable dosage form and the active ingredient in the dosage form have been found to comprise a surprisingly low concentration of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, which is represented by Formula (II):
llllnnõ
O N
N (II).
In some embodiments, the stable dosage form comprises about 0.0001 to about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, as defined by the International Conference on Harmonization (ICH) guidelines, for example after storage for one, two or three months of storage at 40 C and 75% relative humidity. In some embodiments, the stable dosage form comprises less than about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, for example after storage for one, two or three months of storage at 40 C and 75% relative humidity. In some embodiments, the stable dosage form comprises about 0.0001 to about 0.1% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, for example, after storage for one, two or three months of storage at 40 C and 75% relative humidity.
In some preferred embodiments, the stable dosage form comprises about 0.001 to about 0.2 wt.%, about 0.01 to about 0.2 wt.%, about 0.0001 to about 0.15 wt.%, about 0.001 to about 0.15 wt.%, about 0.01 to about 0.15 wt.%, about 0.001 to about 0.1 wt.%, about 0.01 to about 0.1 wt.%, about 0.01 to about 0.08 wt.%, or even about 0.001 to about 0.08 wt.% of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, for example, after storage for one, two, three, four, five or six months of storage at 40 C
and 75%
relative humidity. In some embodiments, the stable dosage form comprises about 0.01 to about 0.08 wt.% (e.g., about 0.001 to about 0.08 wt.%) of (1S, 5R) 1-phenyl-3-azabicyclo [3 - 1 -0] hexane-2-one, for example, after storage for one, two, three, four, five or six months of storage at 40 C and 75% relative humidity.
Preparation of the Stable Dosage Form The stable dosage forms of levomilnacipran can be prepared by any suitable process. In some preferred embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution that comprises (or consists essentially of or consists of) levomilnacipran, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) (e.g., a dehydrated alcohol such as 200-proof ethanol) and optionally a binder and an anti-adherent or lubricant, to form a levomilnacipran composition. In some embodiments, the dosage forms of levomilnacipran are then coated to render them sustained-release dosage forms by contacting the levomilnacipran composition with a solution that comprises a release controlling agent, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) (e.g., a dehydrated alcohol such as 200-proof ethanol) and optionally a plasticizer, an anti-adherent or glidant.
In some preferred embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution that comprises levomilnacipran, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water), a binder, and an anti-adherent or lubricant, to form a levomilnacipran composition. In some embodiments, the dosage forms of levomilnacipran are then coated to render them sustained-release dosage forms by contacting the levomilnacipran composition with a solution that comprises a release controlling agent, a plasticizer, an anti-adherent or glidant, and a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with levomilnacipran and optionally a binder, an anti-adherent or lubricant, and/or a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) to form a levomilnacipran composition (e.g., a levomilnacipran core or levomilnacipran beads or granules). In some embodiments, the dosage forms of levomilnacipran are then coated to render them sustained-release dosage forms by contacting the levomilnacipran composition with a release controlling agent and optionally a plasticizer, an anti-adherent or lubricant; and/or a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution that comprises levomilnacipran, a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water) and optionally a binder and an anti-adherent (or lubricant) to form a levomilnacipran composition (e.g., a core, bead or granule comprising levomilnacipran). In some embodiments, the method further comprises coating the levomilnacipran composition with a solution that comprises (or consists essentially of or consists of) a release controlling agent and optionally a plasticizer, an anti-adherent or lubricant; and/or a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the stable dosage forms are prepared by a method comprising contacting an inert substrate or filler with a solution comprising levomilnacipran, a binder, an anti-adherent or lubricant, and a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some embodiments, the contacting step comprises layering the inert substrate with a drug layering solution that consists essentially of levomilnacipran, a binder, an anti-adherent (or lubricant) and a solvent (e.g., a solvent comprising less than 5 wt.%, less than 4 wt.%, less than 3 wt.%, less than 2 wt.%, less than 1 wt.%, less than 0.8 wt.%, less than 0.5 wt.%, or even less than 0.1 wt.% of water).
In some preferred embodiments, the contacting step (e.g., drug layering step) is performed by a Wurster process (e.g., within a Wurster apparatus) or the like.
In some preferred embodiments, the coating step is performed by a Wurster process (e.g., within a Wurster apparatus) or the like. In some preferred embodiments, the combining step and the contacting steps are both performed by a Wurster process or the like.
The process for determining the relative percentages of levomilnacipran and other isomers of 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide (e.g., 1R,2S 2-(amino methyl)-N,N-diethyl-l-phenyl cyclopropane carboxamide) in the active pharmaceutical ingredient can be performed using any suitable method, preferably by reverse phase high performance liquid chromatograph (RP HPLC) (for example, with a UV detection at 220 nm).
Components of the stable dosage forms The stable dosage form can comprise any therapeutically effective amount of levomilnacipran. In some embodiments, the stable dosage form comprises about 5 to about 200 mg of levomilnacipran. In some embodiments, the stable dosage form comprises about 10 to about 180 mg of levomilnacipran. In some embodiments, the stable dosage form comprises about 20 to about 150 mg of levomilnacipran. In some embodiments, the stable dosage form comprises about 20 to about 120 mg of levomilnacipran. For example, the stable dosage form can comprise about 20 mg, about 40 mg, about 50 mg, about 60 mg, about 80 mg, about 100 mg, 120 mg, or about 240 mg of levomilnacipran. In this regard, the stable dosage form can comprise any suitable weight percentage of levomilnacipran relative to other components of the dosage form.
For example, the stable dosage form can comprise about 35 to about 65% by weight (e.g., about 35 to about 60 wt.%, about 35 to about 55 wt.%, about 40 to about 55 wt.%, or about 40 to about 50 wt.%) of levomilnacipran.
The stable dosage form of levomilnacipran also comprises an inert substrate or filler. In some preferred embodiments, the stable dosage form comprises an inert substrate that comprises sugar for example sucrose (e.g., sugar spheres).
Other suitable inert substrates or fillers include, for example, isomalt, dicalcium phosphate dihydrate, calcium sulfate, lactose, mannitol, sorbitol, cellulose, microcrystalline cellulose, kaolin, sodium chloride, dry starch, hydrolyzed starches, pre-gelatinized starch, silicone dioxide, titanium oxide, magnesium aluminum silicate, or a mixture thereof.
The stable dosage form can comprise any suitable amount of the inert substrate or filler (e.g., sugar spheres). In some embodiments, the stable dosage form comprises about 15 to about 45% by weight of the inert substrate or filler. In some embodiments, the stable dosage form comprises about 20 to about 40 wt.% of the inert substrate or filler. In some embodiments, the stable dosage form comprises about 25 to about 40 wt.% of the inert substrate or filler. In some embodiments, the stable dosage form comprises about 30 to about 40 wt.% of the inert substrate or filler In some embodiments, the stable dosage form comprises about 35 to about 40 wt.% of the inert substrate or filler.
The stable dosage form can comprise sugar spheres in any suitable size. In some embodiments, the stable dosage form comprises sugar spheres having a size of about 20 to about 50 mesh. In some embodiments, the stable dosage form comprises sugar spheres having a size of approximately about 25 to about 45 mesh. In some embodiments, the stable dosage form comprises sugar spheres having a size of about 25 to about 40 mesh.
In some preferred embodiments, the stable dosage form comprises sugar spheres having a size of approximately about 30 to about 40 mesh (for example, about 30 to about 35 mesh). For example, the stable dosage form may comprise about 30 to about 40 wt.%
(e.g., about 35 to about 40 wt.%) of sugar spheres having a size of about 30 to about 40 mesh.
The stable dosage form also comprises a binder in some preferred embodiments, for example polyvinyl pyrrolidone (e.g., Povidone K30). Other suitable binders include, for example, starch, polyvinyl alcohol, pre-gelatinized starch, gelatin, sucrose, glucose, dextrose, lactose, sorbitol, polyethylene glycol, waxes, natural and synthetic gums such as acacia, tragacanth, sodium alginate, hydroxypropylmethylcellulose, hydroxypropylcellulose, ethylcellulose, veegum, and synthetic polymers such as acrylic acid and methacrylic acid copolymers, methacrylic acid copolymers, methyl methacrylate copolymers, aminoalkyl methacrylate copolymers, polyacrylic acid/polymethacrylic acid, or a mixture thereof.
The stable dosage form can comprise any suitable amount of the binder (e.g., PVP). In some embodiments, the stable dosage form comprises about 0.1 to about 15%
by weight of a binder. In some embodiments, the stable dosage form comprises about 1 to about 12% by weight of a binder. In some embodiments, the stable dosage form comprises about 1 to about 10% by weight of a binder. In some embodiments, the stable dosage form comprises about 2 to about 10% by weight of a binder.
In some preferred embodiments, the stable dosage form comprises about 3 to about 10% by weight of a binder (e.g., PVP). In some embodiments, the stable dosage form comprises about 4 to about 10% by weight of the binder. In some embodiments, the stable dosage form comprises about 2 to about 8% by weight of the binder. In some embodiments, the stable dosage form comprises about 4 to about 8% by weight of the binder. In some embodiments, the stable dosage form comprises about 5 to about 7% by weight of the binder.
The stable dosage form also comprises an anti-adherent or lubricant in some preferred embodiments, for example, talc. Other suitable anti-adherents or lubricants include, for example, magnesium stearate, calcium stearate, stearic acid, glycerol behenate, polyethylene glycol, talc, mineral oil, sodium stearyl fumarate or mixtures thereof.
The stable dosage form can comprise any suitable amount of the lubricant or anti-adherent (for example, talc). In some embodiments, the stable dosage form comprises about 0.1 to about 15% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 1 to about 12% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 2 to about 10% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 3 to about 10% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 4 to about 10%
by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 4 to about 8% by weight of the lubricant or anti-adherent. In some embodiments, the stable dosage form comprises about 5 to about 8% by weight of the lubricant or anti-adherent.
In some preferred embodiments, the stable dosage form comprises about 4 to about 7.5% by weight of the lubricant or anti-adherent. In some preferred embodiments, the stable dosage form comprises about 5 to about 7% by weight of the lubricant or anti-adherent.
In some embodiments, the stable dosage form is a sustained-release (SR) dosage form and comprises a release controlling agent, polymeric agent or coating polymer (e.g., ethyl cellulose) which substantially contributes to sustaining the release of levomilnacipran from the dosage form. Other suitable release controlling agents include, for example, a cellulose and cellulose derivative, wax, carbomer, polyalkylene polyol, polycarbophil, methacrylic acid derivative, gelatin, gum, polyethylene oxide, and polyvinyl pyrrolidone, or mixtures thereof. In some embodiments, the release controlling agent, polymeric additive or coating polymer is selected from ethyl cellulose, hydroxypropyl cellulose, hydroxyethyl cellulose, hydroxymethyl cellulose, hydroxypropyl methyl cellulose, hydroxypropyl methyl cellulose acetate succinate, hydroxypropylmethyl cellulose phthalate, methylcellulose, cellulose acetate, cellulose acetate phthalate, cellulose acetate trimellitate and carboxymethylcellulose sodium;
acrylic acid polymers and copolymers (preferably formed from acrylic acid, methacrylic acid, methyl acrylate, ethyl acrylate, methyl methacrylate and/or ethyl methacrylate), and other methacrylic resins that are commercially available under the trade name EudragitTM
(Rohm Pharma; Westerstadt, Germany), including EudragitTM L30D-55 and L100-55, EudragitTM, EudragitTM and EudragitTM NE, RL and RS; vinyl polymers and copolymers such as polyvinyl pyrrolidone, vinyl acetate, vinyl acetate phthalate, vinyl acetate crotonic acid copolymer, and ethylene-vinyl acetate copolymer; enzymatically degradable polymers such as azo polymers, pectin, chitosan, amylose and guar gum; zein and shellac, or mixtures thereof.
The stable dosage form can comprise any suitable amount of the release controlling agent, polymeric agent or coating polymer (e.g., ethyl cellulose).
The stable dosage form preferably comprises about 5 to about 15% by weight of the release controlling agent, polymeric agent or coating polymer. However, n some embodiments, the stable dosage form comprises about 2 to about 20% by weight of a release controlling agent, polymeric agent or coating polymer. In some embodiments, the stable dosage form comprises about 5 to about 12% by weight of a release controlling agent, polymeric agent or coating polymer. In some embodiments, the stable dosage form comprises about 8 to about 12% by weight of a release controlling agent, polymeric agent or coating polymer. In some embodiments, the stable dosage form comprises about 8 to about 11%
by weight of a release controlling agent, polymeric agent or coating polymer.
In some embodiments, the stable dosage form comprises about 8 to about 10% by weight of a release controlling agent, polymeric agent or coating polymer.
The stable dosage form also comprises a plasticizer in some preferred embodiments, for example triethyl citrate. Other suitable plasticizers include, for example, polyethylene glycol, propylene glycol, triacetin, dimethyl phthalate, diethyl phthalate, dibutyl phthalate, dibutyl sebacate, tributyl citrate, triethyl acetyl citrate, glycerol monostearate, castor oil, acetylated monoglycerides, or a mixture thereof.
The stable dosage form can comprise any suitable amount of the plasticizer (for example, triethyl citrate). In some embodiments, the stable dosage form comprises about 0.1 to about 10% by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 0.5 to about 8% by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 0.5 to about 5% by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 1 to about 5%
by weight of the plasticizer. In some embodiments, the stable dosage form comprises about 1 to about 3% by weight of the plasticizer.
In addition, the stable dosage form of levomilnacipran can comprise any additional excipients or additives in some embodiments, such as plasticizers, pigments, colorants, stabilizing agents, glidants, or the like.
In some preferred embodiments, the dosage form comprises about 30 wt.% to about 65 wt.% (e.g., about 40 wt.% to about 60 wt.%, about 45 wt.% to about 60 wt.% or even about 50 wt.% to about 60 wt.%) of levomilnacipran (or an active ingredient comprising at least 98% by weight or even substantially pure levomilnacipran);
about 25 wt.% to about 55 wt.% (e.g., about 30 wt.% to about 45 wt.% or even about 30 wt.% to about 40 wt.%) of an inert substrate or filler; about 2 wt.% to about 12 wt.%
(e.g., about 4 wt.% to about 10 wt.% or even about 4 wt.% to about 8 wt.%) of a binder; and about 0.5 wt.% to about 10 wt.% (e.g., about 1 wt.% to about 8 wt.%, about 1 wt.% to about 5 wt.%
or even about 2 wt.% to about 5 wt.%) of an anti-adherent or lubricant.
In some preferred embodiments, the dosage form comprises about 45 wt.% to about 60 wt.% of levomilnacipran (or an active ingredient comprising at least 98% by weight or even substantially pure levomilnacipran); about 30 wt.% to about 45 wt.% of an inert substrate or filler; about 4 wt.% to about 10 wt.% of a binder; and about 1 wt.%
to about 5 wt.% of an anti-adherent or lubricant.
In some preferred embodiments, the dosage form comprises about 50 wt.% to about 60 wt.% of levomilnacipran (or an active ingredient comprising at least 98% by weight or even substantially pure levomilnacipran); about 30 wt.% to about 40 wt.% of an inert substrate or filler; about 4 wt.% to about 8 wt.% of a binder; and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); and about 0.1 to about 4 wt.%
(e.g., about 1 to about 3 wt.%) of a plasticizer (e.g., triethyl citrate).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
and about 0.1 to about 4 wt.% (e.g., about 1 to about 3 wt.%) of a plasticizer (e.g., triethyl citrate).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
and about 0.1 to about 4 wt.% (e.g., about 1 to about 3 wt.%) of a plasticizer (e.g., triethyl citrate).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); and about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
and about 5-
10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose);
and about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose); and about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose).
In some preferred embodiments, the stable dosage form comprises about 35 to about 60% by weight (e.g., about 35 to about 55 wt.% or about 40 to about 55 wt.%) of levomilnacipran; about 20 to about 45% by weight (e.g., about 20 to about 40 wt.%, about 25 to about 40 wt.% or about 25 to 35 wt.%) of an inert substrate or filler (e.g., sugar spheres); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.% or about 4 to about 8 wt.%) of a binder (for example, PVP); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.%, about 4 to about 8 wt.% or about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc); about 1-20% by weight (e.g., about 5 to about 15 wt.% or about 8 to about 12 wt.%) of a release controlling agent (for example, ethyl cellulose); and about 0.1 to about 10% by weight (e.g., about 0.1 to about 5 wt.% or about 1 to about 5 wt.% or about 1 to about 3 wt.%) of a plasticizer (for example, triethyl citrate).
In some preferred embodiments, the stable dosage form comprises about 35 to about 60% by weight (e.g., about 35 to about 55 wt.% or about 40 to about 55 wt.%) of levomilnacipran; about 20 to about 45% by weight (e.g., about 20 to about 40 wt.%, about 25 to about 40 wt.% or about 25 to 35 wt.%) of an inert substrate (e.g., sugar substrate) (e.g., about 30-35 mesh sugar spheres); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.% or about 4 to about 8 wt.%) of PVP (e.g., Povidone K30); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.%, about 3 to about 8 wt.%, about 4 to about 8 wt.% or about 4 to about 7 wt.%) of talc; about 1-20%
by weight (e.g., about 5 to about 15 wt.% or about 8 to about 12 wt.%) of ethyl cellulose;
and about 0.1 to about 10% by weight (e.g., about 0.1 to about 5 wt.% or about 1 to about 5 wt.% or about 1 to about 3 wt.%) of triethyl citrate.
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 25 to about 40 wt.% of sugar spheres (e.g., about 30-35 mesh sugar spheres); about 2 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of PVP (e.g., Povidone K30); about 2 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of talc; about 5 to about 15 wt.% of ethyl cellulose;
about 0.1 to about 5 wt.% (e.g., about 1 to about 5 wt.%) of triethyl citrate.
The stable dosage forms can comprise beads or granules (e.g., microgranules or other like core) of levomilnacipran that are coated with release controlling agent in any suitable thickness to achieve a desired pK profile. In some embodiments, for example, the stable dosage form is a capsule that contains beads or granules (or similar core), wherein the beads or granules (or similar core) are coated with a coating composition comprising a release controlling agent (and optionally a plasticizer, anti-adherent or lubricant, and/or a solvent) having any desired average thickness. For example, the coating composition can be applied to the beads or granules (or similar core) with an average thickness of about 1 to about 100 microns (e.g., about 5 to about 75 microns, about 5 to about 60 microns, about 5 to about 50 microns, about 5 to about 40 microns, about 5 to about 30 microns, about 10 to about 30 microns, about 15 to about 30 microns, about 20 to about 30 microns, about 25 to about 35 microns, or even about 25 to about 35 microns).
In some preferred embodiments, for example, the stable dosage form comprises coated beads or granules (or similar core) of levomilnacipran wherein the coating comprises one or more release controlling agents (e.g., ethyl cellulose) and wherein the average thickness of the coating on the beads or granules (or similar core) is about 20 to about 35 microns (e.g., about 20 to about 30 microns). For example, the dosage form can be a bead-, granule- or microgranule-filled capsule wherein the beads, granules or microgranules (or similar core) are coated with a coating composition (e.g., comprising ethyl cellulose) at an average thickness of about 20 to about 30 microns (e.g., approximately 25 microns).
In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 400 to about 900 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 500 to about 800 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 600 to about 800 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 600 to about 750 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 650 to about 850 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of less than about 1000 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of less than about 900 microns.
The invention also provides a method for using the stable dosage form of levomilnacipran in the manufacture of a medicament for the treatment of a disorder that can be managed by inhibition of 5-HT and NE reuptake, for example, anxiety disorders or depression (e.g., major depressive disorder).
In some embodiments, the stable dosage form is loaded into a capsule (e.g., an HPMC or gelatin capsule). For example, in some preferred embodiments, the stable dosage form is loaded into an HPMC capsule. Such an HPMC capsule can then be packaged in bottles or canisters with or without a desiccant (e.g., about 0.01 to about 2 grams, about 0.01 to about 1 gram or even about 0.01 to about 0.8 grams of desiccant).
In some preferred embodiments, the stable dosage form is contained within HPMC
capsules and packaged without a desiccant. In some preferred embodiments, the stable dosage form is contained within HPMC capsules and packaged with a desiccant.
In some embodiments, the stable dosage form is contained within gelatin capsules and packaged without a desiccant. In some embodiments, the stable dosage form is contained within gelatin capsules and packaged with a desiccant..
Dissolution Rate of the stable dosage forms The stable dosage forms of levomilnacipran have been found to provide desirable dissolution rates following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of at least about 80% (e.g., at least 80%) after about 6 hours to about 16 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 12 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 60% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 55% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 50% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 45% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 40% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 20% to about 60% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 25%
to about 55% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 30% to about 50%
after about 2 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 65% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 60%
after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 80% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 45% to about 75% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 70% after about 4 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 75% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70%
after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 95% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 50% to about 90% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 60% to about 85% after about 6 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate of about 60% to about 80% after about 6 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 95% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 65%
to about 90% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 85%
after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 85% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 80% after about 8 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 12 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 12 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 75% to about 95% after about 12 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate of about 80% to about 95% after about 12 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 80%
to about 90% after about 12 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of at least about 80% (e.g., at least 80%) after about 6 hours to about 16 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm (for example, after entry into 1000 mL
of deionized water at a temperature of 37 C and subjected to USP apparatus II at 75 rpm, wherein levomilnacipran is quantified using HPLC with a UV detector at a wavelength of 220 nm). In some embodiments, the stable dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 60% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 55% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 50% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 45% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 40% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 20% to about 60% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 25% to about 55% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 30% to about 50% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 65% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 60% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 80% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 45% to about 75% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 70% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 75% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 95% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 50% to about 90% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 60% to about 85% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 60%
to about 80% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 95% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 90% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 65%
to about 85% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 85% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 80% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 75%
to about 95% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 80% to about 95% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 80% to about 90% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form of levomilnacipran achieves the discussed dissolution rates after storage of the dosage form for one, two, or even three months at 40 C and 75% relative humidity (RH).
Pharmacokinetic (pK) Performance of the stable dosage forms The stable dosage forms provide sustained release of levomilnacipran over an extended period of time upon entering a use environment and are expected to achieve a desirable pK profile upon administration to human patients. In some embodiments, the stable dosage forms may provide (i.e., are expected to achieve) a therapeutic blood plasma level of levomilnacipran over approximately a twenty-four hour period, for example after single administration. For example, in some embodiments, the stable dosage forms may release levomilnacipran for about 4 hours to about 24 hours (e.g., for about 5 to about 24 hours, or even for about 6 hours to about 24 hours) following entry of the dosage form into a use environment.
In some embodiments, the stable dosage form may provide a mean Tmax (average time to maximum plasma concentration) of at least 1 hour following administration (e.g., single administration) to a patient. In some embodiments, the stable dosage form may provide a mean Tmax (average time to maximum plasma concentration) of at least 2 hours following administration (e.g., single administration) to a patient. In some embodiments, the stable dosage form may provide a mean Tmax (average time to maximum plasma concentration) of at least 3 hours following administration (e.g., single administration) to a patient. In some embodiments, the stable dosage form may provide a mean Tmax of at least 3.5 hours. Preferably, the stable dosage form of the present invention may provide a mean Tmax of at least 4 hours. For example, the stable dosage form may provide a mean Tmax of at least 4.5 hours.
In some embodiments, the dosage form may provide a mean Tmax of at least 5 hours. In some embodiments, the dosage form may provide a mean Tmax of at least 5.5 hours. In some embodiments, the dosage form may provide a mean Tmax of at least 6 hours. The stable dosage form can also provide a mean Tmax of about 4 hours to about 12 hours. For example, the stable dosage form can provide a mean Tmax of about hours to about 10 hours. In some embodiments, the stable dosage form may provide a mean Tmax of about 4.5 hours to about 12 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4.5 hours to about 10 hours. In some embodiments, the dosage form may provide a mean Tmax of about 5 hours to about hours. In some embodiments, the dosage form may provide a mean Tmax of about 5 hours to about 10 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4 hours to about 8 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4.5 hours to about 8.5 hours. In some embodiments, the dosage form may provide a mean Tmax of about 5 hours to about 8 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4 hours to about hours.
In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 20,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 15,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 10,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 1000 to about 9000 ng. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 5,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 2500 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 500 to about 2200 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 700 to about 2500 ng hr/mL.
In some embodiments, the dosage form may provide a mean AUCO-oc of about 700 to about 2200 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 800 to about 2200 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 700 to about 2300 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1000 to about 2000 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1000 to about 1800 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1100 to about 1800 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1200 to about 1700 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1300 to about 1700 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1300 to about 1650 ng hr/mL.
The average maximum plasma concentration (Cmax) provided by the stable dosage forms can be modified (e.g., without substantially affecting the Tmax of the dosage form) by changing the strength of the dosage form. In some embodiments, the dosage form may provide a mean Cmax of less than about 200 ng/ml following administration (e.g., single administration) to a patient. In some embodiments, the dosage form may provide a mean Cmax of less than about 180 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 170 ng/ml.
In some embodiments, the dosage form may provide a mean Cmax of less than about 160 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 150 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 140 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 130 ng/ml.
In some embodiments, the dosage form may provide a mean Cmax of less than about 120 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 110 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 100 ng/ml. In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 250 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 200 ng/mL.
In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 180 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 30 and about 140 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 40 and about 140 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 150 ng/mL.
The stable dosage forms have also been found, in some embodiments, to provide a mean half life (TI/2) of at least about 6 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 7 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 8 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 9 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 10 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 11 hours.
In some embodiments, the dosage form may provide a mean T1/2 of at least about 12 hours. In some embodiments, the dosage may provide a mean T1/2 of about 6 hours to about 24 hours. In some embodiments, the dosage may provide a mean T1/2 of about 6 hours to about 18 hours. In some embodiments, the dosage may provide a mean T1/2 of about 7 hours to about 18 hours. In some embodiments, the dosage may provide a mean T1/2 of about 8 hours to about 24 hours. In some embodiments, the dosage may provide a mean T1/2 of about 8 hours to about 18 hours.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean AUC0_,c, between about 1000 and about 9000 ng hr/mL.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean Cmax between about 50 and about 350 ng/ml.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean Tmax between about 5 and 12 hours.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean T1/2 between about 9 hours and about 20 hours.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean AUC0_,c, between about 1000 and about 9000 ng hr/mL, a mean Cmax between about 50 and about 350 ng/ml, a mean Tmax between about 5 and 12 hours, and a mean T1/2 between about 9 hours and about 20 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 200 ng/ml, a mean AUC0_,,, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 180 ng/ml, a mean AUC0_,c, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 160 ng/ml, a mean AUC0_,c, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 150 ng/ml, a mean AUC0_,,, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 140 ng/ml, a mean AUC0_,c, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 140 ng/ml, a mean AUC0_,c, of less than about 2200 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 180 ng/ml, a mean AUC0_,c, of less than about 2200 ng hr/mL and a mean Tmax of at least about 5 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 180 ng/ml, a mean AUC0_,,, of less than about 2200 ng hr/mL and a mean Tmax of at least about 6 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_,c, of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 25 to about 175 ng/ml, a mean AUC0_,c, of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about to about 150 ng/ml, a mean AUC0_,,, of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
25 In some embodiments, the stable dosage form may provide a mean Cmax of about 30 to about 120 ng/ml, a mean AUC0_,c, of about 500 to about 2500 hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about to about 200 ng/ml, a mean AUC0_,,, of about 600 to about 2200 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 5 10 to about 200 ng/ml, a mean AUC0_,c, of about 800 to about 2100 ng hr/mL
and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_,c, of about 900 to about 2100 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
10 In some embodiments, the stable dosage form may provide a mean Cmax of about 30 to about 150 ng/ml, a mean AUC0_,c, of about 600 to about 2200 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 30 to about 120 ng/ml, a mean AUC0_,,, of about 600 to about 2200 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_'c' of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 8 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_'c' of about 500 to about 2500 ng hr/mL and a mean Tmax between about 5 to about 8 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 25 to about 175 ng/ml, a mean AUC0_,,, of about 600 to about 2200 ng hr/mL ng hr/mL and a mean Tmax between about 4 to about 9 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 30 to about 150 ng/ml, a mean AUC0_'c' of about 800 to about 2100 ng hr/mL ng hr/mL and a mean Tmax between about 4 to about 9 hours.
In some embodiments, a dosage form is provided, wherein the dosage form may provide an in vivo plasma profile with a mean Cmax of less than about 125 ng/ml, a mean AUC0_. of less than about 1000 to about 2200 ng hr/mL and a mean Tmax of at least about 4 hours.
Methods of Treatment Using the stable dosage forms The present invention also provides methods for treating a disease, disorder or condition that can be managed by inhibition (e.g., double inhibition and/or selective inhibition) of 5-HT and NE reuptake, for example, anxiety disorders or depression (e.g., major depressive disorder (MDD)) in a mammal (e.g., human) by administering the stable dosage form to a patient in need thereof.
In some embodiments, a method is provided for treating or preventing depression (e.g., atypical depression or MDD), anxiety (e.g., generalized anxiety disorder) or fatigue associated with depression or anxiety in a patient in need thereof by administering the stable dosage form of levomilnacipran to said patient. In some embodiments, a method is provided for treating or preventing major depressive disorder (MDD) (e.g., acute MDD
or atypical MDD) in a patient in need thereof by administering the stable dosage form of levomilnacipran to said patient. In some embodiments, a method is provided for treating or preventing MDD with unresolved, concomitant or accompanying fatigue in a patient in need thereof by administering the stable dosage form of levomilnacipran to said patient.
In some embodiments, the stable dosage form of levomilnacipran is used to treat or prevent relapse of MDD in a patient in need thereof by administering the dosage form to said patient. In some embodiments, the stable dosage form is used to treat or prevent fatigue (e.g., fatigue associated with MDD or other form of depression) in a patient in need thereof by administering the dosage form to said patient. In some embodiments, the stable dosage form is used to treat or prevent sexual dysfunction (e.g., erectile dysfunction) in a patient in need thereof by administering the dosage form to said patient.
In some embodiments, the stable dosage form is used to treat or prevent pain associated with depression (e.g., MDD) in a patient in need thereof by administering the dosage form to said patient.
In some embodiments, the stable dosage form of the present invention is used to treat or prevent melancholia, dysthymia, somnolence, cognitive impairment, sleep disorders and/or hyperlipidemia associated (or concomitant) with depression (e.g., MDD) in a patient in need thereof by administering the stable dosage form to said patient.
In some embodiments, a method is provided for treating or preventing neuropathic pain (e.g., diabetic polyneuropathic pain (DPNP)) in a patient in need thereof, wherein the method comprises administering an effective amount of the stable dosage form of levomilnacipran to the patient.
Through administration of the stable dosage form of levomilnacipran, there is provided a method for obtaining a flattened drug plasma concentration to time profile, thereby affording a tighter plasma therapeutic range control than can be obtained with multiple daily dosing. In other words, a method is provided for eliminating the sharp peaks and troughs in blood plasma drug levels induced by multiple daily dosing with conventional immediate release formulations of levomilnacipran. In essence, the plasma levels of levomilnacipran rise after administration of the stable dosage forms of this invention for several hours and then begin to fall through a protracted, substantially linear decrease from the peak plasma level for the remainder of an approximately twenty-four hour period, maintaining at least a threshold therapeutic level of levomilnacipran during the entire period.
The following examples are merely illustrative of the present invention and should not be construed as limiting the scope of the invention in any way as many variations and equivalents that are encompassed by the present invention will become apparent to those skilled in the art upon reading the present disclosure.
EXAMPLES
Example 1: Preparation of a Dosage Form of Levomilnacipran Beads of levomilnacipran were prepared by preheating sugar spheres (approximately 30-35 mesh) and layering the preheated sugar spheres with a drug layer solution for about 3.5 hours via a Wurster process to form drug-loaded beads.
The drug layer solution included levomilnacipran, Povidone K30, talc and a dehydrated alcohol.
The drug-loaded beads were dried in the fluid bed for about 30 minutes and sieved to yield immediate-release levomilnacipran beads (approx. 540 mg/g) which comprised approximately the concentrations of components shown in Table 4:
Table 4 Formulation Components w/w kg/Batch Levomilnacipran 54 30 Sugar Spheres 20 Povidone K30 6 3 Talc 3 2 Dehydrated alcohol' - -Total 100 55 Eliminated during the manufacturing process The levomilnacipran beads were then preheated and coated with a dispersion solution via a Wurster process. The dispersion solution comprised ethyl cellulose N22, triethyl citrate, talc and a dehydrated alcohol. The coated beads were carefully cured in the fluid bed and screened to yield sustained release beads of levomilnacipran (approx.
460 mg/g) prior to filling into capsules. The sustained release levomilnacipran beads comprised approximately the concentrations of components shown in Table 5:
Table 5 Formulation Components w/w kg/Batch Levomilnacipran Beads 85 51 Ethyl cellulose N22 10 6 Triethyl citrate 2 1.2 Talc 3 1.8 Dehydrated alcohol' g.s. g.s.
Total 100 60 i Eliminated during the manufacturing process Example 2: Stability of the Dosage Form Prepared in Example 1 The stability of the dosage form of levomilnacipran prepared in Example 1 was assessed following storage of the dosage form in two different types of capsules (namely, hard gelatin capsules and HPMC capsules) for three months at 40 C and 75%
relative humidity (RH).
Table 6 shows the approximate concentrations of impurities that were found within the hard gelatin capsules of the stable dosage form of levomilnacipran following three months of storage.
Table 6 Impurities Concentration (1S, 5R) 1-phenyl-3-azabicyclo [3-1-0] hexane-2-one Approx. 0.06%
Total unknown related substances Less than appox. 0.05%
Total all related substances Approx. 0.06%
Table 7 shows the approximate concentrations of impurities that were found within HPMC capsules of the stable dosage form of levomilnacipran.
Table 7 Impurities Concentration (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one Less than approx. 0.05%
Total unknown related substances Less than approx. 0.05%
Total all related substances Less than 0.05%
Example 3: Dissolution Rates of Dosage Form Prepared in Example 1 The dissolution rates of the stable dosage form of levomilnacipran prepared in Example 1 was evaluated in 1000 rnL of deionized water at 37 C using USP
apparatus II
at 75 rpm. Quantification of levomilnacipran was determined using I-IPLC with a L7V
detector at a wavelength of 220 nm.
The dissolution profile of the stable dosage form prepared in Example 1 (and loaded into an HPMC capsule containing no desiccant) is shown in Figure 1 and in Table 8.
The dissolution profile of the stable dosage form prepared in Example 1 was also determined after storing the dosage form for one, two and three months at 40 C
and 75%
relative humidity (RH), wherein the dosage form was loaded into HPMC capsules (containing 1 gram or no desiccant), as is shown in Table 8 and in Figures 1-5.
In particular, Figure 1 shows the dissolution rate for the stable dosage form of levomilnacipran after no storage, wherein the dosage form is loaded into an HPMC
capsule that contains no desiccant. Figure 2 shows the dissolution rate for the stable dosage form of levomilnacipran after 1 month of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC capsule that contains no desiccant.
Figure 3 shows the dissolution rate for the stable dosage form of levomilnacipran after 2 months of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC
capsule that contains no desiccant. Figure 4 shows the dissolution rate for the stable dosage form of levomilnacipran after 3 months of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC capsule that contains no desiccant. Figure 5 shows the dissolution rate for the stable dosage form of levomilnacipran after 3 months of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC capsule that contains 1 gram of desiccant.
Table 8 1 month 2 months 3 months 3 months Initial storage storage storage storage (no (no (no (no (1 g desiccant) desiccant) desiccant) desiccant) desiccant) Time Average Average Average Average Average (hrs) % Release % Release % Release % Release % Release 0.5 0 1 0 1 0 1.0 5 9 12 14 8 2.0 31 33 37 39 35 4.0 56 56 59 60 57 6.0 68 67 70 71 69 8.0 76 75 77 77 77 10.0 82 81 83 82 82 12.0 86 84 86 86 86 16.0 92 90 92 91 92 24.0 98 97 98 97 99 Example 4 - X-Ray Powder Diffractometry (XRD) Analysis of an Active Ingredient Comprising Substantially Pure Levomilnacipran A sample of an active ingredient comprising at least 98% by weight of levomilnacipran hydrochloride was loaded onto a deep aluminum holder and exposed to CuKa radiation (40kV x 40 mA) in a wide-angle bench-top X-ray diffractometer (Model D8, Bruker AXS Inc., Madison WI). The instrument was operated in the step-scan mode in increments of 0.05 20. The angular range was 5 to 40 20, and the scan rate was 0.15 20/min. The data collection and analyses were performed with commercially available software.
Peak positions for the XRD pattern in Figure 6 are provided in Table 1.
Table 1 2-Theta d(,A) 2-Theta d(,A) 6.0 14.8 22.4 4.0 12.0 7.4 24.1 3.7 12.4 7.1 24.6 3.6 14.2 6.2 24.8 3.6 17.4 5.1 28.8 3.1 18.2 4.9 30.7 2.9 20.1 4.4 32.7 2.7 21.1 4.2 35.2 2.5 21.6 4.1 Example 5 - X-Ray Powder Diffractometry (XRD) Analysis of the Immediate-Release Levomilnacipran Beads Prepared in Example 1 IR Levomilnacipran beads prepared in Example 1 were loaded onto a deep aluminum holder and exposed to CuKa radiation (40kV x 40 mA) in a wide-angle bench-top X-ray diffractometer (Model D8, Bruker AXS Inc., Madison WI). The instrument was operated in the step-scan mode in increments of 0.05 20. The angular range was 5 to 40 20, and the scan rate was 0.15 20/min. The data collection and analyses were performed with commercially available software.
Peak positions for the XRD pattern in Figure 7 are provided in Table 2.
Table 2 2-Theta d(,A) 2-Theta d(,A) 2.3 39.2 20.0 4.4 5.9 14.9 21.7 4.1 9.5 9.3 22.4 4.0
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of a binder (e.g., PVP); about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose);
and about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose).
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 3 to about 7 wt.% (e.g., about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc);
about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose); and about 5-10.5% by weight (e.g., about 6 to about 10 wt.%) of a release controlling agent (for example, ethyl cellulose).
In some preferred embodiments, the stable dosage form comprises about 35 to about 60% by weight (e.g., about 35 to about 55 wt.% or about 40 to about 55 wt.%) of levomilnacipran; about 20 to about 45% by weight (e.g., about 20 to about 40 wt.%, about 25 to about 40 wt.% or about 25 to 35 wt.%) of an inert substrate or filler (e.g., sugar spheres); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.% or about 4 to about 8 wt.%) of a binder (for example, PVP); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.%, about 4 to about 8 wt.% or about 4 to about 7 wt.%) of an anti-adherent or lubricant (for example, talc); about 1-20% by weight (e.g., about 5 to about 15 wt.% or about 8 to about 12 wt.%) of a release controlling agent (for example, ethyl cellulose); and about 0.1 to about 10% by weight (e.g., about 0.1 to about 5 wt.% or about 1 to about 5 wt.% or about 1 to about 3 wt.%) of a plasticizer (for example, triethyl citrate).
In some preferred embodiments, the stable dosage form comprises about 35 to about 60% by weight (e.g., about 35 to about 55 wt.% or about 40 to about 55 wt.%) of levomilnacipran; about 20 to about 45% by weight (e.g., about 20 to about 40 wt.%, about 25 to about 40 wt.% or about 25 to 35 wt.%) of an inert substrate (e.g., sugar substrate) (e.g., about 30-35 mesh sugar spheres); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.% or about 4 to about 8 wt.%) of PVP (e.g., Povidone K30); about 1 to about 15% by weight (e.g., about 2 to about 12 wt.%, about 3 to about 10 wt.%, about 3 to about 9 wt.%, about 3 to about 8 wt.%, about 4 to about 8 wt.% or about 4 to about 7 wt.%) of talc; about 1-20%
by weight (e.g., about 5 to about 15 wt.% or about 8 to about 12 wt.%) of ethyl cellulose;
and about 0.1 to about 10% by weight (e.g., about 0.1 to about 5 wt.% or about 1 to about 5 wt.% or about 1 to about 3 wt.%) of triethyl citrate.
In some preferred embodiments, the stable dosage form comprises 40 to about 55 wt.% (e.g., about 40 to about 50 wt.%) of levomilnacipran; about 25 to about 40 wt.% of sugar spheres (e.g., about 30-35 mesh sugar spheres); about 2 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of PVP (e.g., Povidone K30); about 2 to about 10 wt.%
(e.g., about 4 to about 8 wt.%) of talc; about 5 to about 15 wt.% of ethyl cellulose;
about 0.1 to about 5 wt.% (e.g., about 1 to about 5 wt.%) of triethyl citrate.
The stable dosage forms can comprise beads or granules (e.g., microgranules or other like core) of levomilnacipran that are coated with release controlling agent in any suitable thickness to achieve a desired pK profile. In some embodiments, for example, the stable dosage form is a capsule that contains beads or granules (or similar core), wherein the beads or granules (or similar core) are coated with a coating composition comprising a release controlling agent (and optionally a plasticizer, anti-adherent or lubricant, and/or a solvent) having any desired average thickness. For example, the coating composition can be applied to the beads or granules (or similar core) with an average thickness of about 1 to about 100 microns (e.g., about 5 to about 75 microns, about 5 to about 60 microns, about 5 to about 50 microns, about 5 to about 40 microns, about 5 to about 30 microns, about 10 to about 30 microns, about 15 to about 30 microns, about 20 to about 30 microns, about 25 to about 35 microns, or even about 25 to about 35 microns).
In some preferred embodiments, for example, the stable dosage form comprises coated beads or granules (or similar core) of levomilnacipran wherein the coating comprises one or more release controlling agents (e.g., ethyl cellulose) and wherein the average thickness of the coating on the beads or granules (or similar core) is about 20 to about 35 microns (e.g., about 20 to about 30 microns). For example, the dosage form can be a bead-, granule- or microgranule-filled capsule wherein the beads, granules or microgranules (or similar core) are coated with a coating composition (e.g., comprising ethyl cellulose) at an average thickness of about 20 to about 30 microns (e.g., approximately 25 microns).
In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 400 to about 900 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 500 to about 800 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 600 to about 800 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 600 to about 750 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of about 650 to about 850 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of less than about 1000 microns. In some embodiments, the stable dosage form is in the form of beads or granules (e.g., coated beads or granules) which have an average diameter of less than about 900 microns.
The invention also provides a method for using the stable dosage form of levomilnacipran in the manufacture of a medicament for the treatment of a disorder that can be managed by inhibition of 5-HT and NE reuptake, for example, anxiety disorders or depression (e.g., major depressive disorder).
In some embodiments, the stable dosage form is loaded into a capsule (e.g., an HPMC or gelatin capsule). For example, in some preferred embodiments, the stable dosage form is loaded into an HPMC capsule. Such an HPMC capsule can then be packaged in bottles or canisters with or without a desiccant (e.g., about 0.01 to about 2 grams, about 0.01 to about 1 gram or even about 0.01 to about 0.8 grams of desiccant).
In some preferred embodiments, the stable dosage form is contained within HPMC
capsules and packaged without a desiccant. In some preferred embodiments, the stable dosage form is contained within HPMC capsules and packaged with a desiccant.
In some embodiments, the stable dosage form is contained within gelatin capsules and packaged without a desiccant. In some embodiments, the stable dosage form is contained within gelatin capsules and packaged with a desiccant..
Dissolution Rate of the stable dosage forms The stable dosage forms of levomilnacipran have been found to provide desirable dissolution rates following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of at least about 80% (e.g., at least 80%) after about 6 hours to about 16 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 12 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 60% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 55% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 50% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 45% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 40% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 20% to about 60% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 25%
to about 55% after about 2 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 30% to about 50%
after about 2 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 65% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 60%
after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 80% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 45% to about 75% after about 4 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 70% after about 4 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 75% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70%
after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 95% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 50% to about 90% after about 6 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 60% to about 85% after about 6 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate of about 60% to about 80% after about 6 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 95% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 65%
to about 90% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 85%
after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 85% after about 8 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 80% after about 8 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 12 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 12 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 75% to about 95% after about 12 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate of about 80% to about 95% after about 12 hours following entry into a use environment. In some embodiments, the stable dosage form provides a dissolution rate of about 80%
to about 90% after about 12 hours following entry into a use environment.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of at least about 80% (e.g., at least 80%) after about 6 hours to about 16 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm (for example, after entry into 1000 mL
of deionized water at a temperature of 37 C and subjected to USP apparatus II at 75 rpm, wherein levomilnacipran is quantified using HPLC with a UV detector at a wavelength of 220 nm). In some embodiments, the stable dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 60% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 55% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 50% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 45% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 40% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 20% to about 60% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 25% to about 55% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 30% to about 50% after about 2 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 65% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 60% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 80% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 45% to about 75% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 70% after about 4 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 90% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 80% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 75% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 70% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 40% to about 95% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 50% to about 90% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 60% to about 85% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 60%
to about 80% after about 6 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 85% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 95% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 65% to about 90% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 65%
to about 85% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 85% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 70% to about 80% after about 8 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form provides a dissolution rate (e.g., a single phase dissolution rate) of less than about 95% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of less than about 90% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 75%
to about 95% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 80% to about 95% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP
apparatus II at 75 rpm. In some embodiments, the stable dosage form provides a dissolution rate of about 80% to about 90% after about 12 hours following entry into deionized water at a temperature of about 37 C and subjected to USP apparatus II at 75 rpm.
In some embodiments, the stable dosage form of levomilnacipran achieves the discussed dissolution rates after storage of the dosage form for one, two, or even three months at 40 C and 75% relative humidity (RH).
Pharmacokinetic (pK) Performance of the stable dosage forms The stable dosage forms provide sustained release of levomilnacipran over an extended period of time upon entering a use environment and are expected to achieve a desirable pK profile upon administration to human patients. In some embodiments, the stable dosage forms may provide (i.e., are expected to achieve) a therapeutic blood plasma level of levomilnacipran over approximately a twenty-four hour period, for example after single administration. For example, in some embodiments, the stable dosage forms may release levomilnacipran for about 4 hours to about 24 hours (e.g., for about 5 to about 24 hours, or even for about 6 hours to about 24 hours) following entry of the dosage form into a use environment.
In some embodiments, the stable dosage form may provide a mean Tmax (average time to maximum plasma concentration) of at least 1 hour following administration (e.g., single administration) to a patient. In some embodiments, the stable dosage form may provide a mean Tmax (average time to maximum plasma concentration) of at least 2 hours following administration (e.g., single administration) to a patient. In some embodiments, the stable dosage form may provide a mean Tmax (average time to maximum plasma concentration) of at least 3 hours following administration (e.g., single administration) to a patient. In some embodiments, the stable dosage form may provide a mean Tmax of at least 3.5 hours. Preferably, the stable dosage form of the present invention may provide a mean Tmax of at least 4 hours. For example, the stable dosage form may provide a mean Tmax of at least 4.5 hours.
In some embodiments, the dosage form may provide a mean Tmax of at least 5 hours. In some embodiments, the dosage form may provide a mean Tmax of at least 5.5 hours. In some embodiments, the dosage form may provide a mean Tmax of at least 6 hours. The stable dosage form can also provide a mean Tmax of about 4 hours to about 12 hours. For example, the stable dosage form can provide a mean Tmax of about hours to about 10 hours. In some embodiments, the stable dosage form may provide a mean Tmax of about 4.5 hours to about 12 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4.5 hours to about 10 hours. In some embodiments, the dosage form may provide a mean Tmax of about 5 hours to about hours. In some embodiments, the dosage form may provide a mean Tmax of about 5 hours to about 10 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4 hours to about 8 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4.5 hours to about 8.5 hours. In some embodiments, the dosage form may provide a mean Tmax of about 5 hours to about 8 hours. In some embodiments, the dosage form may provide a mean Tmax of about 4 hours to about hours.
In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 20,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 15,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 10,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 1000 to about 9000 ng. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 5,000 ng hr/mL. In some embodiments, the stable dosage form may provide a mean AUCO-oc (plasma concentration of levomilnacipran over time) of about 500 to about 2500 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 500 to about 2200 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 700 to about 2500 ng hr/mL.
In some embodiments, the dosage form may provide a mean AUCO-oc of about 700 to about 2200 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 800 to about 2200 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 700 to about 2300 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1000 to about 2000 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1000 to about 1800 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1100 to about 1800 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1200 to about 1700 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1300 to about 1700 ng hr/mL. In some embodiments, the dosage form may provide a mean AUCO-oc of about 1300 to about 1650 ng hr/mL.
The average maximum plasma concentration (Cmax) provided by the stable dosage forms can be modified (e.g., without substantially affecting the Tmax of the dosage form) by changing the strength of the dosage form. In some embodiments, the dosage form may provide a mean Cmax of less than about 200 ng/ml following administration (e.g., single administration) to a patient. In some embodiments, the dosage form may provide a mean Cmax of less than about 180 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 170 ng/ml.
In some embodiments, the dosage form may provide a mean Cmax of less than about 160 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 150 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 140 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 130 ng/ml.
In some embodiments, the dosage form may provide a mean Cmax of less than about 120 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 110 ng/ml. In some embodiments, the dosage form may provide a mean Cmax of less than about 100 ng/ml. In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 250 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 200 ng/mL.
In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 180 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 30 and about 140 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 40 and about 140 ng/mL. In some embodiments, the dosage form may provide a mean Cmax between about 20 and about 150 ng/mL.
The stable dosage forms have also been found, in some embodiments, to provide a mean half life (TI/2) of at least about 6 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 7 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 8 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 9 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 10 hours. In some embodiments, the dosage form may provide a mean T1/2 of at least about 11 hours.
In some embodiments, the dosage form may provide a mean T1/2 of at least about 12 hours. In some embodiments, the dosage may provide a mean T1/2 of about 6 hours to about 24 hours. In some embodiments, the dosage may provide a mean T1/2 of about 6 hours to about 18 hours. In some embodiments, the dosage may provide a mean T1/2 of about 7 hours to about 18 hours. In some embodiments, the dosage may provide a mean T1/2 of about 8 hours to about 24 hours. In some embodiments, the dosage may provide a mean T1/2 of about 8 hours to about 18 hours.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean AUC0_,c, between about 1000 and about 9000 ng hr/mL.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean Cmax between about 50 and about 350 ng/ml.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean Tmax between about 5 and 12 hours.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean T1/2 between about 9 hours and about 20 hours.
In some preferred embodiments, the stable dosage form is a modified-release dosage form and provides a mean AUC0_,c, between about 1000 and about 9000 ng hr/mL, a mean Cmax between about 50 and about 350 ng/ml, a mean Tmax between about 5 and 12 hours, and a mean T1/2 between about 9 hours and about 20 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 200 ng/ml, a mean AUC0_,,, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 180 ng/ml, a mean AUC0_,c, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 160 ng/ml, a mean AUC0_,c, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 150 ng/ml, a mean AUC0_,,, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 140 ng/ml, a mean AUC0_,c, of less than about 2500 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 140 ng/ml, a mean AUC0_,c, of less than about 2200 ng hr/mL and a mean Tmax of at least about 4 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 180 ng/ml, a mean AUC0_,c, of less than about 2200 ng hr/mL and a mean Tmax of at least about 5 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of less than about 180 ng/ml, a mean AUC0_,,, of less than about 2200 ng hr/mL and a mean Tmax of at least about 6 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_,c, of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 25 to about 175 ng/ml, a mean AUC0_,c, of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about to about 150 ng/ml, a mean AUC0_,,, of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
25 In some embodiments, the stable dosage form may provide a mean Cmax of about 30 to about 120 ng/ml, a mean AUC0_,c, of about 500 to about 2500 hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about to about 200 ng/ml, a mean AUC0_,,, of about 600 to about 2200 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 5 10 to about 200 ng/ml, a mean AUC0_,c, of about 800 to about 2100 ng hr/mL
and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_,c, of about 900 to about 2100 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
10 In some embodiments, the stable dosage form may provide a mean Cmax of about 30 to about 150 ng/ml, a mean AUC0_,c, of about 600 to about 2200 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide a mean Cmax of about 30 to about 120 ng/ml, a mean AUC0_,,, of about 600 to about 2200 ng hr/mL and a mean Tmax between about 4 to about 10 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_'c' of about 500 to about 2500 ng hr/mL and a mean Tmax between about 4 to about 8 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 10 to about 200 ng/ml, a mean AUC0_'c' of about 500 to about 2500 ng hr/mL and a mean Tmax between about 5 to about 8 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 25 to about 175 ng/ml, a mean AUC0_,,, of about 600 to about 2200 ng hr/mL ng hr/mL and a mean Tmax between about 4 to about 9 hours.
In some embodiments, the stable dosage form may provide an in vivo plasma profile with a mean Cmax of about 30 to about 150 ng/ml, a mean AUC0_'c' of about 800 to about 2100 ng hr/mL ng hr/mL and a mean Tmax between about 4 to about 9 hours.
In some embodiments, a dosage form is provided, wherein the dosage form may provide an in vivo plasma profile with a mean Cmax of less than about 125 ng/ml, a mean AUC0_. of less than about 1000 to about 2200 ng hr/mL and a mean Tmax of at least about 4 hours.
Methods of Treatment Using the stable dosage forms The present invention also provides methods for treating a disease, disorder or condition that can be managed by inhibition (e.g., double inhibition and/or selective inhibition) of 5-HT and NE reuptake, for example, anxiety disorders or depression (e.g., major depressive disorder (MDD)) in a mammal (e.g., human) by administering the stable dosage form to a patient in need thereof.
In some embodiments, a method is provided for treating or preventing depression (e.g., atypical depression or MDD), anxiety (e.g., generalized anxiety disorder) or fatigue associated with depression or anxiety in a patient in need thereof by administering the stable dosage form of levomilnacipran to said patient. In some embodiments, a method is provided for treating or preventing major depressive disorder (MDD) (e.g., acute MDD
or atypical MDD) in a patient in need thereof by administering the stable dosage form of levomilnacipran to said patient. In some embodiments, a method is provided for treating or preventing MDD with unresolved, concomitant or accompanying fatigue in a patient in need thereof by administering the stable dosage form of levomilnacipran to said patient.
In some embodiments, the stable dosage form of levomilnacipran is used to treat or prevent relapse of MDD in a patient in need thereof by administering the dosage form to said patient. In some embodiments, the stable dosage form is used to treat or prevent fatigue (e.g., fatigue associated with MDD or other form of depression) in a patient in need thereof by administering the dosage form to said patient. In some embodiments, the stable dosage form is used to treat or prevent sexual dysfunction (e.g., erectile dysfunction) in a patient in need thereof by administering the dosage form to said patient.
In some embodiments, the stable dosage form is used to treat or prevent pain associated with depression (e.g., MDD) in a patient in need thereof by administering the dosage form to said patient.
In some embodiments, the stable dosage form of the present invention is used to treat or prevent melancholia, dysthymia, somnolence, cognitive impairment, sleep disorders and/or hyperlipidemia associated (or concomitant) with depression (e.g., MDD) in a patient in need thereof by administering the stable dosage form to said patient.
In some embodiments, a method is provided for treating or preventing neuropathic pain (e.g., diabetic polyneuropathic pain (DPNP)) in a patient in need thereof, wherein the method comprises administering an effective amount of the stable dosage form of levomilnacipran to the patient.
Through administration of the stable dosage form of levomilnacipran, there is provided a method for obtaining a flattened drug plasma concentration to time profile, thereby affording a tighter plasma therapeutic range control than can be obtained with multiple daily dosing. In other words, a method is provided for eliminating the sharp peaks and troughs in blood plasma drug levels induced by multiple daily dosing with conventional immediate release formulations of levomilnacipran. In essence, the plasma levels of levomilnacipran rise after administration of the stable dosage forms of this invention for several hours and then begin to fall through a protracted, substantially linear decrease from the peak plasma level for the remainder of an approximately twenty-four hour period, maintaining at least a threshold therapeutic level of levomilnacipran during the entire period.
The following examples are merely illustrative of the present invention and should not be construed as limiting the scope of the invention in any way as many variations and equivalents that are encompassed by the present invention will become apparent to those skilled in the art upon reading the present disclosure.
EXAMPLES
Example 1: Preparation of a Dosage Form of Levomilnacipran Beads of levomilnacipran were prepared by preheating sugar spheres (approximately 30-35 mesh) and layering the preheated sugar spheres with a drug layer solution for about 3.5 hours via a Wurster process to form drug-loaded beads.
The drug layer solution included levomilnacipran, Povidone K30, talc and a dehydrated alcohol.
The drug-loaded beads were dried in the fluid bed for about 30 minutes and sieved to yield immediate-release levomilnacipran beads (approx. 540 mg/g) which comprised approximately the concentrations of components shown in Table 4:
Table 4 Formulation Components w/w kg/Batch Levomilnacipran 54 30 Sugar Spheres 20 Povidone K30 6 3 Talc 3 2 Dehydrated alcohol' - -Total 100 55 Eliminated during the manufacturing process The levomilnacipran beads were then preheated and coated with a dispersion solution via a Wurster process. The dispersion solution comprised ethyl cellulose N22, triethyl citrate, talc and a dehydrated alcohol. The coated beads were carefully cured in the fluid bed and screened to yield sustained release beads of levomilnacipran (approx.
460 mg/g) prior to filling into capsules. The sustained release levomilnacipran beads comprised approximately the concentrations of components shown in Table 5:
Table 5 Formulation Components w/w kg/Batch Levomilnacipran Beads 85 51 Ethyl cellulose N22 10 6 Triethyl citrate 2 1.2 Talc 3 1.8 Dehydrated alcohol' g.s. g.s.
Total 100 60 i Eliminated during the manufacturing process Example 2: Stability of the Dosage Form Prepared in Example 1 The stability of the dosage form of levomilnacipran prepared in Example 1 was assessed following storage of the dosage form in two different types of capsules (namely, hard gelatin capsules and HPMC capsules) for three months at 40 C and 75%
relative humidity (RH).
Table 6 shows the approximate concentrations of impurities that were found within the hard gelatin capsules of the stable dosage form of levomilnacipran following three months of storage.
Table 6 Impurities Concentration (1S, 5R) 1-phenyl-3-azabicyclo [3-1-0] hexane-2-one Approx. 0.06%
Total unknown related substances Less than appox. 0.05%
Total all related substances Approx. 0.06%
Table 7 shows the approximate concentrations of impurities that were found within HPMC capsules of the stable dosage form of levomilnacipran.
Table 7 Impurities Concentration (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one Less than approx. 0.05%
Total unknown related substances Less than approx. 0.05%
Total all related substances Less than 0.05%
Example 3: Dissolution Rates of Dosage Form Prepared in Example 1 The dissolution rates of the stable dosage form of levomilnacipran prepared in Example 1 was evaluated in 1000 rnL of deionized water at 37 C using USP
apparatus II
at 75 rpm. Quantification of levomilnacipran was determined using I-IPLC with a L7V
detector at a wavelength of 220 nm.
The dissolution profile of the stable dosage form prepared in Example 1 (and loaded into an HPMC capsule containing no desiccant) is shown in Figure 1 and in Table 8.
The dissolution profile of the stable dosage form prepared in Example 1 was also determined after storing the dosage form for one, two and three months at 40 C
and 75%
relative humidity (RH), wherein the dosage form was loaded into HPMC capsules (containing 1 gram or no desiccant), as is shown in Table 8 and in Figures 1-5.
In particular, Figure 1 shows the dissolution rate for the stable dosage form of levomilnacipran after no storage, wherein the dosage form is loaded into an HPMC
capsule that contains no desiccant. Figure 2 shows the dissolution rate for the stable dosage form of levomilnacipran after 1 month of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC capsule that contains no desiccant.
Figure 3 shows the dissolution rate for the stable dosage form of levomilnacipran after 2 months of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC
capsule that contains no desiccant. Figure 4 shows the dissolution rate for the stable dosage form of levomilnacipran after 3 months of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC capsule that contains no desiccant. Figure 5 shows the dissolution rate for the stable dosage form of levomilnacipran after 3 months of storage at 40 C and 75% RH, wherein the dosage form is loaded into an HPMC capsule that contains 1 gram of desiccant.
Table 8 1 month 2 months 3 months 3 months Initial storage storage storage storage (no (no (no (no (1 g desiccant) desiccant) desiccant) desiccant) desiccant) Time Average Average Average Average Average (hrs) % Release % Release % Release % Release % Release 0.5 0 1 0 1 0 1.0 5 9 12 14 8 2.0 31 33 37 39 35 4.0 56 56 59 60 57 6.0 68 67 70 71 69 8.0 76 75 77 77 77 10.0 82 81 83 82 82 12.0 86 84 86 86 86 16.0 92 90 92 91 92 24.0 98 97 98 97 99 Example 4 - X-Ray Powder Diffractometry (XRD) Analysis of an Active Ingredient Comprising Substantially Pure Levomilnacipran A sample of an active ingredient comprising at least 98% by weight of levomilnacipran hydrochloride was loaded onto a deep aluminum holder and exposed to CuKa radiation (40kV x 40 mA) in a wide-angle bench-top X-ray diffractometer (Model D8, Bruker AXS Inc., Madison WI). The instrument was operated in the step-scan mode in increments of 0.05 20. The angular range was 5 to 40 20, and the scan rate was 0.15 20/min. The data collection and analyses were performed with commercially available software.
Peak positions for the XRD pattern in Figure 6 are provided in Table 1.
Table 1 2-Theta d(,A) 2-Theta d(,A) 6.0 14.8 22.4 4.0 12.0 7.4 24.1 3.7 12.4 7.1 24.6 3.6 14.2 6.2 24.8 3.6 17.4 5.1 28.8 3.1 18.2 4.9 30.7 2.9 20.1 4.4 32.7 2.7 21.1 4.2 35.2 2.5 21.6 4.1 Example 5 - X-Ray Powder Diffractometry (XRD) Analysis of the Immediate-Release Levomilnacipran Beads Prepared in Example 1 IR Levomilnacipran beads prepared in Example 1 were loaded onto a deep aluminum holder and exposed to CuKa radiation (40kV x 40 mA) in a wide-angle bench-top X-ray diffractometer (Model D8, Bruker AXS Inc., Madison WI). The instrument was operated in the step-scan mode in increments of 0.05 20. The angular range was 5 to 40 20, and the scan rate was 0.15 20/min. The data collection and analyses were performed with commercially available software.
Peak positions for the XRD pattern in Figure 7 are provided in Table 2.
Table 2 2-Theta d(,A) 2-Theta d(,A) 2.3 39.2 20.0 4.4 5.9 14.9 21.7 4.1 9.5 9.3 22.4 4.0
11.9 7.4 24.5 3.6
12.3 7.2 28.6 3.1 14.1 6.3 30.6 2.9 16.5 5.4 32.7 2.7 17.3 5.1 34.5 2.6 18.1 4.9 Example 6 - X-Ray Powder Diffractometry (XRD) Analysis of the Sustained-Release Dosage Form Prepared in Example 1 A small amount of the sustained-release dosage form prepared in Example 1 was loaded on a deep aluminum holder and exposed to CuKa radiation (40kV x 40 mA) in a wide-angle bench-top X-ray diffractometer (Model D8, Bruker AXS Inc., Madison WI).
The instrument was operated in a step-scan mode in increments of 0.05 20. The angular range was 5 to 40 20, and the scan rate was 0.15 20/min. Data collection and analyses were performed with commercially available software (specifically, DIFFRACp1us XRD
Commander, Bruker-AXS GmbH; and JADE, Materials Data, Inc.).
The XRD pattern for the stable dosage form of levomilnacipran is shown in Figure 7. Peak positions for the XRD pattern in Figure 8 are provided in Table 3.
Table 3 2-Theta d(A) 2-Theta d(A) 6.0 14.7 22.1 4.0 8.3 10.6 22.5 4.0 9.6 9.2 23.6 3.8 12.0 7.4 24.7 3.6 12.8 6.9 25.2 3.5
The instrument was operated in a step-scan mode in increments of 0.05 20. The angular range was 5 to 40 20, and the scan rate was 0.15 20/min. Data collection and analyses were performed with commercially available software (specifically, DIFFRACp1us XRD
Commander, Bruker-AXS GmbH; and JADE, Materials Data, Inc.).
The XRD pattern for the stable dosage form of levomilnacipran is shown in Figure 7. Peak positions for the XRD pattern in Figure 8 are provided in Table 3.
Table 3 2-Theta d(A) 2-Theta d(A) 6.0 14.7 22.1 4.0 8.3 10.6 22.5 4.0 9.6 9.2 23.6 3.8 12.0 7.4 24.7 3.6 12.8 6.9 25.2 3.5
13.1 6.7 26.4 3.4
14.2 6.2 27.5 3.2
15.6 5.7 28.7 3.1
16.4 5.4 30.6 2.9 16.8 5.3 31.0 2.9
17.4 5.1 32.0 2.8
18.3 4.8 32.7 2.7 18.9 4.7 33.5 2.7
19.6 4.5 34.6 2.6
20.0 4.4 36.2 2.5 20.4 4.4 37.3 2.4 20.9 4.2 38.3 2.3
21.6 4.1 Example 7 - Administration of Stable Dosage Forms of Levomilnacipran to Human Patients (Prophetic) The stable dosage forms of levomilnacipran of the present invention can be administered to human patients in the form of capsules that contain 50 mg of levomilnacipran. The capsules may contain microgranules that are coated with about 7.5 wt.% of ethyl cellulose (EC) ("dosage form 1"), about 10 wt.% EC ("dosage form 2") and about 12.5 wt.% EC ("dosage form 3").
Dosage forms 1-3 can be administered to patients after a fasting period of at least about 10 hours. Blood samples can be collected from each patient before administration and at several time points after administration (e.g., at 30 minutes, 1 hour, 2 hours, 3 hours, 4 hours, 5 hours, 6 hours, 7 hours, 8 hours, 10 hours, 12 hours, 24 hours, 48 hours and 72 hours). Plasma samples from each patient can be assayed for levomilnacipran quantification using a validated on-line extraction method (Turbulent Flow Chromatography) coupled with LC/MS-MS detection.
Oral administration of the stable dosage form is expected to yield pharmacokinetic (pK) parameters substantially as shown for any of dosage forms 1-3 in Table 9. In some preferred embodiments, the stable dosage form will yield pK
parameters substantially as shown for dosage form 2. These PK parameters are expressed as geometric mean (geometric CV%) and [range].
Table 9 Dosage Cmax Tmax* AUCo_,c, T1/2 Tlag* F
Form (ng.mL-1) (h) (h.ng.mL-1) (h) (h) (%) 1 83 (23%) 5 1585 (19%) 12(11%) 0.3 107(5%) [53-120] [5-7] [1035-2018] [10-15] [0-0.5] [96-113]
2 70 (25%) 6 1477 (17%) 13 (13%) 0.5 100 (11%) [43-97] [5-7] [1032-1825] [10-15] [0-1] [82-114]
3 58(16%) 7 1331 (15%) 13(14%) 1 89(9%) [42.5-75] [5-8] [967-1592] [10-16.5] [0-1] [73-100]
* - Median value for Tmax and Tlag.
The mean levomilnacipran plasma concentration versus time profiles that may be obtained after single oral administrations (up to 24 hours post dosing) are shown in Figure 9 (log-linear scale expressed as geometric mean).
While the invention has been depicted and described by reference to exemplary embodiments of the invention, such a reference does not imply a limitation on the invention, and no such limitation is to be inferred. The invention is capable of considerable modification, alteration, and equivalents in form and function, as will occur to those ordinarily skilled in the pertinent arts having the benefit of this disclosure.
The depicted and described embodiments of the invention are exemplary only, and are not exhaustive of the scope of the invention. Consequently, the invention is intended to be limited only by the spirit and scope of the appended claims, giving full cognizance to equivalence in all respects.
Dosage forms 1-3 can be administered to patients after a fasting period of at least about 10 hours. Blood samples can be collected from each patient before administration and at several time points after administration (e.g., at 30 minutes, 1 hour, 2 hours, 3 hours, 4 hours, 5 hours, 6 hours, 7 hours, 8 hours, 10 hours, 12 hours, 24 hours, 48 hours and 72 hours). Plasma samples from each patient can be assayed for levomilnacipran quantification using a validated on-line extraction method (Turbulent Flow Chromatography) coupled with LC/MS-MS detection.
Oral administration of the stable dosage form is expected to yield pharmacokinetic (pK) parameters substantially as shown for any of dosage forms 1-3 in Table 9. In some preferred embodiments, the stable dosage form will yield pK
parameters substantially as shown for dosage form 2. These PK parameters are expressed as geometric mean (geometric CV%) and [range].
Table 9 Dosage Cmax Tmax* AUCo_,c, T1/2 Tlag* F
Form (ng.mL-1) (h) (h.ng.mL-1) (h) (h) (%) 1 83 (23%) 5 1585 (19%) 12(11%) 0.3 107(5%) [53-120] [5-7] [1035-2018] [10-15] [0-0.5] [96-113]
2 70 (25%) 6 1477 (17%) 13 (13%) 0.5 100 (11%) [43-97] [5-7] [1032-1825] [10-15] [0-1] [82-114]
3 58(16%) 7 1331 (15%) 13(14%) 1 89(9%) [42.5-75] [5-8] [967-1592] [10-16.5] [0-1] [73-100]
* - Median value for Tmax and Tlag.
The mean levomilnacipran plasma concentration versus time profiles that may be obtained after single oral administrations (up to 24 hours post dosing) are shown in Figure 9 (log-linear scale expressed as geometric mean).
While the invention has been depicted and described by reference to exemplary embodiments of the invention, such a reference does not imply a limitation on the invention, and no such limitation is to be inferred. The invention is capable of considerable modification, alteration, and equivalents in form and function, as will occur to those ordinarily skilled in the pertinent arts having the benefit of this disclosure.
The depicted and described embodiments of the invention are exemplary only, and are not exhaustive of the scope of the invention. Consequently, the invention is intended to be limited only by the spirit and scope of the appended claims, giving full cognizance to equivalence in all respects.
Claims (23)
1. A stable dosage form comprising levomilnacipran or a pharmaceutically acceptable salt thereof.
2. A stable dosage form comprising an active ingredient that comprises at least 98%
by weight of levomilnacipran or pharmaceutically acceptable salt thereof.
by weight of levomilnacipran or pharmaceutically acceptable salt thereof.
3. The stable dosage form of claim 2, wherein the dosage form comprises an X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 ~ 0.2 degrees 2.SLZERO..
4. The stable dosage form of claim 3, wherein the XRD pattern further comprises a characteristic peak at 32.7 ~ 0.2 degrees 2.SLZERO..
5. The stable dosage form of claim 3, wherein the XRD pattern further comprises a characteristic peak at 6.0 ~ 0.2 degrees 2.SLZERO..
6. The stable dosage form of claim 2, wherein the dosage form comprises a XRD
pattern that comprises characteristic peaks at 6.0, 12.0 and 20.1 ~ 0.2 degrees 2.SLZERO..
pattern that comprises characteristic peaks at 6.0, 12.0 and 20.1 ~ 0.2 degrees 2.SLZERO..
7. The stable dosage form of claim 2, wherein the dosage form comprises about 0.001% to about 0.5% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one.
8. The stable dosage form of claim 2, wherein the dosage form comprises about 0.001% to about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one.
9. The stable dosage form of claim 2, wherein the dosage form comprises about wt.% to about 60 wt.% of the active ingredient, and about 30 wt.% to about 45 wt.% of an inert substrate or filler.
10. The stable dosage form of claim 2, wherein the dosage form comprises about wt.% to about 60 wt.% the active ingredient; about 30 wt.% to about 45 wt.% of an inert substrate or filler; about 4 wt.% to about 10 wt.% of a binder; and about 1 wt.% to about wt.% of an anti-adherent or lubricant.
11. The stable dosage form of claim 2, wherein the dosage form comprises about wt.% to about 60 wt.% of the active ingredient; about 30 wt.% to about 40 wt.%
of an inert substrate or filler; about 4 wt.% to about 8 wt.% of a binder; and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
of an inert substrate or filler; about 4 wt.% to about 8 wt.% of a binder; and about 1 wt.% to about 5 wt.% of an anti-adherent or lubricant.
12. The stable dosage form of claim 9, wherein the dosage form is an immediate-release oral dosage form.
13. The stable dosage form of claim 2, wherein the dosage form comprises about 40%
to about 55% by weight of levomilnacipran or pharmaceutically acceptable salt thereof, about 5% to about 15% by weight of a release controlling agent, about 25% to about 40%
by weight of an inert substrate, about 3% to about 10% by weight of a binder, about 3%
to about 10% by weight of an anti-adherent, and about 0.1% to about 5% by weight of a plasticizer.
to about 55% by weight of levomilnacipran or pharmaceutically acceptable salt thereof, about 5% to about 15% by weight of a release controlling agent, about 25% to about 40%
by weight of an inert substrate, about 3% to about 10% by weight of a binder, about 3%
to about 10% by weight of an anti-adherent, and about 0.1% to about 5% by weight of a plasticizer.
14. The stable dosage form of claim 13, wherein the dosage form is a modified-release oral dosage form.
15. The dosage form of claim 2, wherein the dosage form provides a dissolution rate of at least about 80% after about 6 hours to about 16 hours following entry into a use environment.
16. A stable dosage form comprising an active ingredient that comprises substantially pure levomilnacipran or pharmaceutically acceptable salt thereof, and about 0.01% to about 0.2% by weight of (1S, 5R) 1-phenyl-3-azabicyclo[3-1-0] hexane-2-one, wherein the dosage form comprises an X-ray powder diffraction (XRD) pattern that comprises characteristic peaks at 12.0, 20.1 and 22.5 ~ 0.2 degrees 2.SLZERO..
17. The stable dosage form of claim 16, wherein the dosage form comprises about 45 wt.% to about 60 wt.% of the active ingredient; and about 4 wt.% to about 10 wt.% of a binder.
18. A method for treating major depressive disorder comprising administering the stable dosage form of claim 1 to a patient in need thereof.
19. A method for treating major depressive disorder comprising administering the stable dosage form of claim 2 to a patient in need thereof.
20. A method for treating major depressive disorder comprising administering the stable dosage form of claim 16 to a patient in need thereof.
21. A method for preparing the stable dosage form of claim 1, wherein the method comprises contacting an inert substrate with levomilnacipran or a pharmaceutically acceptable salt thereof and a dehydrated alcohol.
22. A method for preparing the stable dosage form of claim 2, wherein the method comprises contacting an inert substrate with levomilnacipran or a pharmaceutically acceptable salt thereof and a dehydrated alcohol.
23. A method for preparing the stable dosage form of claim 16, wherein the method comprises contacting an inert substrate with levomilnacipran or a pharmaceutically acceptable salt thereof and a dehydrated alcohol.
Applications Claiming Priority (5)
Application Number | Priority Date | Filing Date | Title |
---|---|---|---|
US29489810P | 2010-01-14 | 2010-01-14 | |
US61/294,898 | 2010-01-14 | ||
US12/941,293 | 2010-11-08 | ||
US12/941,293 US8865937B2 (en) | 2009-11-06 | 2010-11-08 | Crystalline forms of (1S,2R)-2-(amino methyl)-N,N-diethyl-1-phenyl cyclopropane carboxamide |
PCT/US2011/021315 WO2011088331A1 (en) | 2010-01-14 | 2011-01-14 | Stable dosage forms of levomilnacipran |
Publications (1)
Publication Number | Publication Date |
---|---|
CA2790933A1 true CA2790933A1 (en) | 2011-07-21 |
Family
ID=44304671
Family Applications (1)
Application Number | Title | Priority Date | Filing Date |
---|---|---|---|
CA2790933A Abandoned CA2790933A1 (en) | 2010-01-14 | 2011-01-14 | Stable dosage forms of levomilnacipran |
Country Status (4)
Country | Link |
---|---|
EP (1) | EP2536688A4 (en) |
JP (1) | JP2013517290A (en) |
CA (1) | CA2790933A1 (en) |
WO (1) | WO2011088331A1 (en) |
Families Citing this family (2)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
FR2978350B1 (en) * | 2011-07-28 | 2013-11-08 | Pf Medicament | LEVOMILNACIPRAN-BASED MEDICINAL PRODUCT FOR FUNCTIONAL REHABILITATION AFTER ACUTE NEUROLOGICAL ACCIDENT |
CN110711185A (en) * | 2018-07-11 | 2020-01-21 | 北京万全德众医药生物技术有限公司 | Levomilnacipran sustained-release capsule |
Family Cites Families (10)
Publication number | Priority date | Publication date | Assignee | Title |
---|---|---|---|---|
FR2752732B1 (en) * | 1996-08-28 | 1998-11-20 | Pf Medicament | EXTENDED RELEASE GALENIC FORM OF MILNACIPRAN |
US20040034101A1 (en) * | 2001-11-05 | 2004-02-19 | Cypress Bioscience, Inc. | Treatment and prevention of depression secondary to pain (DSP) |
AR042806A1 (en) * | 2002-12-27 | 2005-07-06 | Otsuka Pharma Co Ltd | COMBINATION OF CARBOSTIRILE DERIVATIVES AND INHIBITORS OF SEROTONINE REABSORTION FOR THE TREATMENT OF ANIMO DISORDERS |
PT1601349E (en) * | 2003-02-14 | 2008-10-27 | Pf Medicament | Use of the enantiomer (1s, 2r) of milnacipran for the preparation of a medicament |
FR2851163B1 (en) * | 2003-02-14 | 2007-04-27 | USE OF DEXTROGYAN ENANTIOMER OF MILNACIPRAN FOR THE PREPARATION OF A MEDICINAL PRODUCT | |
JP5036029B2 (en) * | 2005-06-10 | 2012-09-26 | 旭化成ファーマ株式会社 | Stabilized milnacipran formulation |
JP2008273867A (en) * | 2007-04-27 | 2008-11-13 | Asahi Kasei Pharma Kk | Preparation for transmucosal administration |
EP2110129A1 (en) * | 2008-04-18 | 2009-10-21 | Pierre Fabre Medicament | Use of enantiomer (1S, 2R) milnacipran hydrochloride for the preventive treatment of suicidal behaviour in depressed patients |
US20100286260A1 (en) * | 2009-05-05 | 2010-11-11 | Forest Laboratories Holdings Ltd. | Milnacipran formulations |
CA2779711C (en) * | 2009-11-06 | 2016-11-01 | Forest Laboratories Holding Limited | Novel crystalline forms of (1s,2r)-2-(amino methyl)-n,n-diethyl-1-phenyl cyclopropane carboxamide |
-
2011
- 2011-01-14 WO PCT/US2011/021315 patent/WO2011088331A1/en active Application Filing
- 2011-01-14 CA CA2790933A patent/CA2790933A1/en not_active Abandoned
- 2011-01-14 JP JP2012549117A patent/JP2013517290A/en active Pending
- 2011-01-14 EP EP11733447.4A patent/EP2536688A4/en not_active Withdrawn
Also Published As
Publication number | Publication date |
---|---|
EP2536688A1 (en) | 2012-12-26 |
EP2536688A4 (en) | 2014-04-02 |
JP2013517290A (en) | 2013-05-16 |
WO2011088331A1 (en) | 2011-07-21 |
Similar Documents
Publication | Publication Date | Title |
---|---|---|
US20180028476A1 (en) | Stable dosage forms of levomilnacipran | |
US20040258749A1 (en) | Oral dosage form for propiverine or its pharmaceutically acceptable salts with an extended release of the active ingredient | |
EP2205279B1 (en) | Pharmaceutical combination of aliskiren and valsartan | |
CA2718639C (en) | Methylphenidate extended release therapeutic drug delivery system | |
KR20090029830A (en) | Pharmaceutical preparation for oral administration with controlled active ingredient release in the small intestine and methods for its production | |
WO2008020286A2 (en) | Pharmaceutical compositions of duloxetine | |
EP2968177A1 (en) | Extended-release topiramate capsules | |
CA2790933A1 (en) | Stable dosage forms of levomilnacipran | |
US20200253901A1 (en) | Stable dosage forms of levomilnacipran | |
US20110130434A1 (en) | Modified release ramipril compositions and uses thereof | |
AU2016255302B2 (en) | Rivastigmine-containing sustained-release pharmaceutical composition | |
US20110150942A1 (en) | Gastro-resistant pharmaceutical oral compositions comprising duloxetine or its pharmaceutically acceptable derivatives | |
AU2006247357B2 (en) | Morphine sulfate formulations | |
US20030091633A1 (en) | Methods and compositions for use of (S)-bisoprolol | |
US20120082718A1 (en) | Morphine Formulations | |
ZA200403764B (en) | Methods and compositions for use of (S)-bisoprolol. | |
AU2002348878A1 (en) | Methods and compositions for use of (S)-bisoprolol |
Legal Events
Date | Code | Title | Description |
---|---|---|---|
EEER | Examination request |
Effective date: 20160114 |
|
FZDE | Discontinued |
Effective date: 20221003 |
|
FZDE | Discontinued |
Effective date: 20221003 |