WO2015123389A1 - Highly purified pharmaceutical grade tasimelteon - Google Patents

Highly purified pharmaceutical grade tasimelteon Download PDF

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Publication number
WO2015123389A1
WO2015123389A1 PCT/US2015/015564 US2015015564W WO2015123389A1 WO 2015123389 A1 WO2015123389 A1 WO 2015123389A1 US 2015015564 W US2015015564 W US 2015015564W WO 2015123389 A1 WO2015123389 A1 WO 2015123389A1
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WO
WIPO (PCT)
Prior art keywords
tasimelteon
impurity
cyclopropyl
dihydrobenzofuran
methyl
Prior art date
Application number
PCT/US2015/015564
Other languages
French (fr)
Inventor
Deepak Phadke
Natalie M. PLATT
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Vanda Pharmaceuticals Inc.
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Priority to EP18207420.3A priority Critical patent/EP3470405A1/en
Priority to EP23167851.7A priority patent/EP4223747A1/en
Priority to EP15708063.1A priority patent/EP3105212A1/en
Priority to JP2016552281A priority patent/JP6921534B2/en
Priority to US15/117,734 priority patent/US10071977B2/en
Application filed by Vanda Pharmaceuticals Inc. filed Critical Vanda Pharmaceuticals Inc.
Publication of WO2015123389A1 publication Critical patent/WO2015123389A1/en
Priority to US16/123,303 priority patent/US10611744B2/en
Priority to US16/800,721 priority patent/US10829465B2/en
Priority to US17/039,795 priority patent/US11203581B2/en
Priority to US17/455,308 priority patent/US11566011B2/en
Priority to US18/149,590 priority patent/US11760740B2/en
Priority to US18/362,073 priority patent/US12049457B2/en
Priority to US18/741,969 priority patent/US20240336584A1/en

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Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D307/00Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom
    • C07D307/77Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom ortho- or peri-condensed with carbocyclic rings or ring systems
    • C07D307/78Benzo [b] furans; Hydrogenated benzo [b] furans
    • C07D307/79Benzo [b] furans; Hydrogenated benzo [b] furans with only hydrogen atoms, hydrocarbon or substituted hydrocarbon radicals, directly attached to carbon atoms of the hetero ring
    • C07D307/81Radicals substituted by nitrogen atoms not forming part of a nitro radical
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61PSPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
    • A61P25/00Drugs for disorders of the nervous system
    • A61P25/20Hypnotics; Sedatives
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D307/00Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom
    • C07D307/77Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom ortho- or peri-condensed with carbocyclic rings or ring systems
    • C07D307/78Benzo [b] furans; Hydrogenated benzo [b] furans
    • C07D307/79Benzo [b] furans; Hydrogenated benzo [b] furans with only hydrogen atoms, hydrocarbon or substituted hydrocarbon radicals, directly attached to carbon atoms of the hetero ring

Definitions

  • the disclosure relates generally to the synthesis of tasimelteon.
  • impurities which may be by-products or degradation products, are analyzed and controlled in order to keep the impurities below pre-set specifications.
  • Tasimelteon N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)- propionamide, is a melatonin agonist useful in the treatment of persons suffering from certain sleep-related disorders.
  • a synthesis of tasimelteon is disclosed, e.g., in Example 2 of US 5,856,529.
  • the end step synthesis in that example comprises reaction of ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanamine with propionyl chloride.
  • Synthesis of the methanamine intermediate is described in Preparation 24 and comprises reaction of ((lR,2R)-2-(2,3- dihydrobenzofuran-4-yl))cyclopropanecarboxaldehyde with hydroxylamine
  • Preparation 18 and comprises palladium catalyzed cyclization of a propenoyl intermediate, specifically, (lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)propenoyl)-2,10- camphorsultam.
  • the invention relates to a process for synthesizing highly purified, pharmaceutical grade tasimelteon, the process comprising: (a) propionylating ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) methanamine or a salt thereof to yield tasimelteon;
  • step (b) crystallizing the tasimelteon produced in step (a);
  • step (c) assaying the crystallized tasimelteon from step (b) for the presence of one or both of Impurity 5 (N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran- 4-yl) cyclopropyl) (propionamido)methyl) cyclopropyl) methyl) propionamide) and Impurity 6 (2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate) ; and
  • the invention relates to a process for preparing a batch of highly purified, pharmaceutical grade tasimelteon, the process comprising: (a) analyzing a batch of tasimelteon synthesized under conditions of Good
  • impurity (ies) that is (are) one or more of:
  • further specifications for continuing to process the tasimelteon are pre-set, e.g., that the tasimelteon is not less than ("NLT") 95.0%, or NLT 98.0% pure (by area under the curve) and/or that the amount of any other single impurity is NMT 0.10 area%.
  • the invention relates to a process for preparing a batch of tasimelteon drug product (i.e., tasimelteon plus excipients) wherein release of a batch of tasimelteon bulk drug substance for use in the manufacture of the tasimelteon drug product is contingent upon the testing and application of acceptance criteria for the amounts of one or more of the following impurities:
  • the invention relates to purified tasimelteon wherein the tasimelteon does not contain any of Impurities 1 through 7 at a
  • such composition does not contain any related-substance impurity (i.e., an impurity that is structurally related to tasimelteon such as degradation products, dimers, etc.) at a concentration of greater than about 0.15% by weight.
  • related-substance impurity i.e., an impurity that is structurally related to tasimelteon such as degradation products, dimers, etc.
  • tasimelteon can result in a plurality of impurities following the end step synthesis.
  • An illustrative synthesis of tasimelteon is a linear process, passing through a methanamine intermediate such as by the process described in US 5,856,529 and involving four purification steps: one purification step for each of three isolated intermediates, as described below, as well as one for the unmilled tasimelteon drug substance.
  • the inventors have discovered that in the synthesis of tasimelteon there are certain impurities that can be formed as both by-products and degradation products, and that these impurities can be controlled or reduced to non-detectable or acceptably detectable levels. Although not desiring to be bound by theory, the inventors have identified some of these impurities on the basis of mass spectrometric, nuclear magnetic resonance spectroscopic and other data. The inventors have found that the impurities can include one or more of:
  • Impurities 1-3 and 5-6 may be by-products of certain steps of the synthesis of tasimelteon, and impurities 4 and 7 may be degradation products.
  • the inventors have also found that in the synthesis of tasimelteon, there are certain additional impurities that can occur as degradation products, reaction byproducts, residual reagents, and residual intermediates. These additional impurities can be controlled or reduced to non-detectable or acceptably detectable levels.
  • impurities can include (+)-dehydroabietylamine, propionyl chloride, propionic acid, ethyl propionate [possibly additional potential degradants of propionyl chloride], ethyl diazoacetate, Intermediates 2, 4, and 5, 4-vinyl-2,3-dihydrobenzofuran (VBF), 4-(2- chloroethyl)-2,3-dihydrobenzofuran (VBF-int-2), benzene, and heavy metals such as As, Al, Fe, Li, Ni, Ru, Pd, Mn, Rh, Cu, and Co.
  • this invention comprises a batch of pharmaceutical grade, highly purified tasimelteon that has been analyzed for the presence of any or each of these impurities and determined to have less than a pre-determined amount of one or more of them.
  • the pre-determined amounts i.e., the pre-set specifications, for these
  • the pre-set specification for Impurities 1-7 and the additional impurities can be 0.15 wt%. In a further embodiment, the pre-set specification can be 0.10 area%, e.g., for unidentified impurities. Additionally, a pre-set specification may include not more than (NMT) lOOppm or NMT 10 ppm of ethyl diazaoacetate (EDA)
  • the impurities are detectable by analytical chemical techniques such as
  • chromatographic and mass spectrometry techniques among others.
  • HPLC, GC, or other chromatography methods can be used, in which case the amount of one or of each of the impurities can be determined on the basis of wt% or of area under the curve.
  • Preparation 18 and comprises palladium catalyzed cyclization of a propenoyl intermediate, specifically, ((lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)propenoyl)-2,10- camphorsultam.
  • An alternative route to the methanamine intermediate or a salt thereof proceeds through (lR,2R)-2-(2,3-dihydrobenzofuran-4- yfjcyclopropanecarboxylate (Intermediate 3) to (lR,2R)-2-(2,3-dihydrobenzofuran-4- yfjcyclopropane-carboxamide (Intermediate 4) and then to Intermediate 5 or a salt thereof.
  • step (b) crystallizing the tasimelteon produced in step (a);
  • step (c) assaying the crystallized tasimelteon from step (b) for the presence of one or both of Impurity 5 (N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran- 4-yl) cyclopropyl) (propionamido)methyl) cyclopropyl) methyl) propionamide) and Impurity 6 (2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate) ; and (d) (i) if the crystallized tasimelteon meets pre-set specifications for Impurity 5 or Impurity 6, or both, then collecting the highly purified, pharmaceutical grade tasimelteon or
  • the propionylating step may comprise contacting ((1R,2R)- 2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methanamine or a salt thereof with a propionyl halide, a propionyl anhydride, a propionyl ester, a propionyl amide, a propionyl imidazolide, or with propionic acid and a dehydrating agent or the product thereof.
  • Water is a byproduct of the coupling of ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanamine with propionic acid to form tasimelteon.
  • the dehydrating agent which is also known as a peptide coupling reagent, is an agent that activates propionic acid toward reaction with ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanamine and consumes the byproduct, water.
  • dehydrating agents include but are not limited to dicyclohexylcarbodiimide (DCC), DCC and an aminopyridine, ⁇ , ⁇ '-carbonyldiimidazole, chlorosilanes, Amberlyst-15,
  • the propionylation may be carried out in the presence of an organic solvent (e.g., ter- butyl methyl ether) and an aqueous base (e.g., NaOH), After the propionylation step and before the crystallizing step, the mixture of tasimelteon may be assayed for the presence of Intermediate 5 (or the free base or other salt thereof) and, if the mixture does not meet pre-set specifications for Intermediate 5 (e.g., not more than 0.15 % or not more than 0.10 %), then repeating step (a) or discarding the mixture.
  • an organic solvent e.g., ter- butyl methyl ether
  • an aqueous base e.g., NaOH
  • the mixture of tasimelteon may be washed with aqueous base and the aqueous layer discarded, after which the washed mixture may be distilled (e.g., in ethanol at up to about 58 °C, and less than about 100 mmHg).
  • the crystallization step may comprise dissolving the tasimelteon by stirring and warming a mixture of the tasimelteon and a C1-C4 alkanol (e.g., about 35 to about 40 °C) and then cooling (e.g., to about 13 to about 17 °C) while stirring.
  • the crystallization step optionally comprises seeding.
  • An illustrative synthesis of tasimelteon in one embodiment, can include the following reaction schemes with a number of intermediates being synthesized first.
  • VBF-int-2 can comprise contacting and reacting 2,3-Bis(2- hydroxyethyl) phenol (Triol) with N,N-dimethylchloromethyleneiminium chloride (the Vilsmeier reagent) in an organic solvent, followed by reacting the resulting N,N'-[(3- hydroxy-l,2-phenylene)-bis(ethane-2,l-diyloxymethylidene)] -bis(N- methylmethanaminium) dichloride (VBF-int-1) with triethylamine in an organic solvent.
  • the Vilsmeier reagent may be generated in situ from N,N-dimethylformamide (DMF) and oxalyl chloride. Said reaction is illustrated in the following scheme:
  • VBF-int-1 (Stage 4)
  • VBF-int-2 (Stage 5)
  • a first reaction mixture can be prepared by slowly adding oxalyl chloride (approximately 2.45-2.55 equiv) to a solution of DMF (approximately 2.45-2.55 equiv) in CH3CN (Acetonitrile (e.g., 16% by weight DMF)) at -10 ⁇ 5 °C while maintaining the batch temperature at -10 ⁇ 5 °C. Stirring may be continued at this temperature for approximately 30-40 min to complete the formation of the Vilsmeier reagent
  • Triol (N,Ndimethylchloromethyleneiminium chloride) in situ.
  • Triol (Stage 3) (1.00 equiv; e.g., 30 kg) is added to the solution of the Vilsmeier reagent in portions through an addition funnel while maintaining the batch temperature at -10 ⁇ 5 °C. Stirring is continued at about -20 to about -5 °C for at least 90 min, until testing via high pressure liquid chromatography (HPLC) indicates that no more than (NMT) 2.0% Triol (Stage 3) remains in solution. If necessary, the mixture can be sampled again at 150 min and tested again for Triol levels. Following this, a solution of Et3N (triethylamine
  • CH3CN e.g., 47% by weight Et3N
  • CH3CN e.g., 47% by weight Et3N
  • the total volume of CH3CN should be approximately 5- 17 L/kg of Triol (Stage 3) input, and in one embodiment may belO L/kg of Triol (Stage 3) input.
  • the mixture may be heated to 55 ⁇ 5 °C for 3-3.5 hr. The mixture may then be cooled to 25 ⁇ 5 °C and stirred for up to four increments of up to approximately 1 hr each until HPLC indicates VBF-int-1 (Stage 4) NMT 2.0 area%.
  • a solution of H3PO4 (8.5% by weight) in aqueous brine (e.g., 5 kg of H3PO4 solution / kg of Triol (Stage 3)) is slowly added to the remaining organic layer. This mixture can be stirred for 30-40 min and settled for 30-40 min. The aqueous layer is removed once more. The organic phase can be washed one or more times with tap water (e.g., 5 L / kg of Triol (Stage 3)) , each time stirring for approximately 30-40 minutes, settling for approximately 30-40 min, and removing the aqueous layer.
  • tap water e.g., 5 L / kg of Triol (Stage 3)
  • the organic layer is distilled at ⁇ 100 torr and less than approximately 40 °C until no more distillate is collected.
  • the batch residue is subjected to short path distillation at 0.1 - 4 torr. Any distillate boiling below 105°C is discarded.
  • the distillate boiling at 105-130 °C is subjected to HPLC analysis. Material meeting a pre-set specification, e.g., VBF-int-2 (Stage 5) present at not less than (NLT) 95.0%, is used directly in the next step.
  • VBF The synthesis of VBF can comprise contacting and reacting 4-(2-Chloroethyl)-2,3- dihydrobenzofuran (VBF-int-2) with tetrabutylammonium hydroxide in the presence of organic solvent. Said reaction is illustrated in the following scheme: VB F-int-2 (Stage 5) 6)
  • tetrabutylammonium hydroxide (0.78 kg / kg of VBF-int-2 (Stage 5)), potassium iodide (0.09 kg / kg of VBF-int-2 (Stage 5)) and VBF-int-2 (from above (Stage 5)) is added to a mixture of TBME (tert-Butyl methyl ether) (5.60 kg / kg of VBFint-2 (Stage 5)) and 45% aqueous NaOH (4.80 kg / kg of VBF-int-2 (Stage 5)).
  • TBME tert-Butyl methyl ether
  • the NaOH, tetrabutylammonium hydroxide and KI charges are in the ranges 7-10, 0.15-0.50 and 0.08-0.10 molar equivalents, respectively.
  • the mixture may be heated to 50 ⁇ 5 °C and stirred for approximately 3-3.5 hr.
  • the mixture is then cooled to 25 ⁇ 5 °C and stirred for up to four increments of NLT 1 hr each until testing via HPLC indicates VBF-int-2 Stage 5) NMT 1.0%.
  • the mixture is settled for 20-30 min and 40-60 L of the aqueous layer is discharged.
  • aqueous HC1 e.g., up to 6.2 kg / kg of VBFint-2 (Stage 5)
  • aqueous HC1 e.g., up to 6.2 kg / kg of VBFint-2 (Stage 5)
  • aqueous NaOH aqueous NaOH
  • the mixture can then be filtered using TBME (1 kg / kg of VBF-int-2 (Stage 5)) to complete the transfer and the filtrate settled for 20-30 minutes.
  • the aqueous layer may then be removed.
  • the synthesis of Intermediate 3 can comprise asymmetric cyclopropanation of 4-vinyl-2,3-dihydrobenzofuran (VBF (Stage 6)) by contacting and reacting it with EDA in the presence of a chiral catalyst.
  • It can also comprise hydrolysis of the ester group of 2-(2,3-dihydrobenzofuran-4-yl)-cyclopropanecarboxylic acid ethyl ester (VEC-int-1 (Stage 7)) followed by polishing resolution of 2-(2,3-dihydrobenzofuran-4-yl)- cyclopropanecarboxylic acid (Intermediate 2 (Stage 8)) with (+)-dehydroabietylamine (DAA) in an organic solvent.
  • Said reaction sequence is illustrated in the following scheme:
  • a lithium diisopropylamide (LDA) solution may be prepared. For instance, a solution of n-butyllithium (0.03 equiv; 1 M in hexanes) is added, slowly, to a solution of
  • a Ru catalyst may be prepared from BTBSC and the LDA solution.
  • the preparation can comprise stirring a mixture of BTBSC (0.02 equiv; e.g., 0.04 M) in THF (tetrahydrofuran) at 25 ⁇ 5 °C for 30-40 min, and then cooling the mixture to 5 ⁇ 5 °C.
  • the LDA solution from above may then be added slowly to this mixture at 5 ⁇ 5 °C and the mixture stirred for approximately 60 min.
  • To the resulting mixture is added, in portions, [Ru(pcymene)Ch]2 (0.02 equiv, assuming 2 equiv Ru / mole of [Ru(p-cymene)Ch]2) .
  • the reactor is purged three times with N2.
  • VBF may undergo cyclopropanation.
  • Toluene e.g., 60 L
  • the mixture is again distilled at ⁇ 100 torr and ⁇ 50°C until about 20 L of residue remains in the reaction vessel.
  • the batch residue is cooled to 30 ⁇ 2 °C, and the Ru catalyst prepared above is added.
  • the Ru catalyst charge can include an amount of
  • the ethyl diazoacetate charge can include
  • VEC-int-1 may undergo a saponification.
  • An illustrative example may include adding 45% aqueous NaOH (4 equiv), 55% aqueous tetrabutylammonium hydroxide (TBAH; 0.45 equiv) and tap water (e.g., 10 L) to the final reaction mixture from the cyclopropanation of VBF. This mixture is then stirred at 50-70 °C for 16-18 hr until HPLC indicates ⁇ 2.0% VEC-int-1 (Stage 7). If the limit is not met, stirring is continued at 50-70 °C for 2-4 hr and the analysis is repeated. Once the limit is met, the mixture is cooled to 25-30 °C.
  • Tap water e.g., 60.0 L
  • TBME e.g., 107.0 kg
  • Phosphoric acid 85% aqueous, e.g., 24.0 kg
  • 10% aqueous NaOH is added to bring the pH into this range.
  • the mixture is then stirred for at least approximately 30 min and settled for another 30-40 min, the aqueous layer being discarded.
  • Tap water e.g., 70.0L
  • This tap water wash may be repeated, for instance three more washes may be utilized.
  • the Intermediate 3 (Stage 9) (DAA salt) may be formed.
  • TBME e.g., 22.9 kg / kg of VBF (Stage 6)
  • ethanol EtOH; anhydrous, e.g., 4.49 kg / kg of VBF (Stage 6)
  • EtOH anhydrous, e.g., 4.49 kg / kg of VBF (Stage 6)
  • the ratio of Intermediate 2 (Stage 8) to TBME may be included in a range of 0.040-0.079 kg Intermediate 2 (Stage 8) / L TBME, and in a further embodiment may comprise a set point of 0.040 kg Intermediate 2 (Stage 8) / L TBME.
  • the ratio of TBME (kg):EtOH (kg) may be 7.78-9.08, and in a further embodiment may be 7.78.
  • (+)-dehydroabietylamine (1.44 equiv) as a 28% wt/wt solution in TBME may be added to the resulting mixture.
  • the (+)-dehydroabietylamine charge may be 1.44-1.76 molar equivalents, and in a further embodiment may be 1.44 molar equivalents.
  • This reaction mixture may be heated to 45- 55 °C and stirred for NLT 20 min, cooled to 25-30 °C in a period of NLT 2 hr and stirred at this temperature for NLT 1 hr, heated to 45-55 °C and stirred for NLT 20 min, cooled to 15-25 °C in a period of NLT 2 hr and stirred for NLT 4 hr, cooled to 0-5 °C in a period of NLT 1 hr and stirred for NLT 1 hr, and the precipitated solid is collected by
  • NLT 99.0 area% and total impurities NMT 2.0% is dried at NMT 80 torr and 60 ⁇ 5 °C for NLT 12 hr until loss on drying (LOD) meets a pre-set specification e.g., LOD NMT 2.0%. Material failing this specification is dried further at NMT 80 torr and 60 ⁇ 5 °C for NLT 6 hr and re-sampled.
  • LOD loss on drying
  • the second process may comprise adding the wet cake to a cooled (e.g., 0-10 °C) mixture of 45% aqueous NaOH (e.g., 3.60 kg/kg of VBF (Stage 6)), tap water (e.g., 11.9 kg/kg of VBF (Stage 6)) and toluene (e.g., 4.49 kg/kg of VBF (Stage 6)), stirring for about 30 min, settling for about 30 min, and phase separation.
  • a cooled (e.g., 0-10 °C) mixture of 45% aqueous NaOH (e.g., 3.60 kg/kg of VBF (Stage 6)), tap water (e.g., 11.9 kg/kg of VBF (Stage 6)) and toluene (e.g., 4.49 kg/kg of VBF (Stage 6) stirring for about 30 min, settling for about 30 min, and phase separation.
  • TBME e.g., 12.0 kg/kg of VBF (Stage 6)
  • VBF VBF
  • the pH of the aqueous layer is adjusted with phosphoric acid (85% aqueous, e.g., 24.0 kg) and, if necessary, 10% aqueous NaOH to a value of 4.0-4.5.
  • phosphoric acid 85% aqueous, e.g., 24.0 kg
  • 10% aqueous NaOH a value of 4.0-4.5
  • the synthesis of Intermediate 4 can comprise liberation of the free carboxylic acid from (li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl) cyclopropanecarboxylic acid (+)- dehydroabietylamine salt (Intermediate 3) followed by conversion via the
  • Intermediate 4 may be synthesized by adding Intermediate 3 (Stage 9) (1 equiv, e.g., 20.0-21.0 kg) to a first reaction mixture of tap water (e.g., 5.2 L / kg of Intermediate 3 (Stage 9)), 45% aqueous NaOH (4 equiv), and toluene (e.g., 1.8 kg / kg of Intermediate 3 (Stage 9)) at 20-30 °C. The mixture is then stirred at 25-30 °C for NLT 30 min and settled for 30-40 min, and the organic layer discarded.
  • Toluene (e.g., 1.8 kg / kg of Intermediate 3 (Stage 9)) is added to the aqueous layer, followed by stirring for NLT 60 min, settling for 30-40 min and discarding the organic layer. The toluene wash can be repeated. Next, sodium chloride (e.g., 0.3 kg / kg of Intermediate 3 (Stage 9)) is added to the remaining aqueous layer. The temperature is adjusted to 15-20 °C. Butyl acetate (e.g., 1.2 kg / kg of Intermediate 3 (Stage 9)) is added. Hydrochloric acid (32% aqueous, 2.9 equiv) is added slowly.
  • sodium chloride e.g., 0.3 kg / kg of Intermediate 3 (Stage 9)
  • Butyl acetate e.g., 1.2 kg / kg of Intermediate 3 (Stage 9)
  • Hydrochloric acid (32% aqueous, 2.9 equiv) is added slowly.
  • the temperature is maintained at 15-20 °C while the mixture is stirred for NLT 60 min and settled for 30-40 min. If the pH of the aqueous layer is more than 3, additional 32% HC1 is added until the pH is less than 3.
  • the layers are separated, and the organic layer is set aside for later use.
  • the aqueous layer is added to butyl acetate (e.g., 1.1 kg / kg of Intermediate 3 (Stage 9)).
  • the temperature is maintained at 15-20 °C while the mixture is stirred for NLT 60 min and settled for 30-40 min.
  • the aqueous layer is discarded.
  • the organic layers are combined and distilled at ⁇ 100 torr and a pot temperature of NMT 82 °C until the batch residue is about 30 L. The distillate is discarded.
  • Butyl acetate (e.g., 0.71 kg / kg of Intermediate 3 (Stage 9) is added to the batch residue. This mixture is distilled at ⁇ 100 torr and a pot temperature of NMT 82 °C until the batch residue is about 30 L. The distillate is discarded. This step is repeated one or two more times until Karl Fischer moisture analysis indicates a value of less than approximately 0.1%.
  • the batch residue is cooled to 15-20 °C.
  • DMF (0.03 equiv) and thionyl chloride (1.3 equiv) are added. The mixture is heated to 50-55 °C, stirred for 1.5-2.0 hr and cooled to 21 ⁇ 4 °C, and analyzed by HPLC.
  • This wet cake is added to a mixture of butyl acetate (e.g., 0.71 kg / kg of Intermediate 3 (Stage 9)) and n-heptane (e.g., 0.3 kg / kg of Intermediate 3 (Stage 9)) at 0-10 °C.
  • the resulting mixture is stirred for 30-40 min at 0-10 °C and then centrifuged at full speed for 20 ⁇ 5 min.
  • the wet cake is analyzed by HPLC to determine if pre-set specifications are met, e.g., Intermediate 4 (Stage 10) NLT 98.0%. If this specification is not met, the wet cake can be added to another mixture of butyl acetate and n-heptane, the stirring and
  • the synthesis of Intermediate 5 can comprise contacting and reacting (li?,2i?)-2-(2,3- dihydrobenzofuran-4- yl)cyclopropanecarboxamide (Intermediate 4) with Lithium aluminum hydride in an organic solvent, followed by aqueous workup and isolation of the resulting amine as its hydrochloride salt. Said reaction is illustrated in the following scheme:
  • Intermediate 5 may be synthesized by the above scheme, wherein the synthesis may include the following procedure.
  • a reactor e.g., SS316
  • refluxing acetone e.g., 100 kg
  • drained e.g., 100 kg
  • dried e.g., 100 kg
  • N 2 gas e.g., N 2 gas
  • the Intermediate 4 (Stage 10) (1.00 equiv) made above and THF e.g., 8 kg / kg of Intermediate 4 (Stage 10) are added to the dry reactor and cooled to -10 °C.
  • LAH Lithium aluminum hydride
  • This mixture is stirred at 65-70 °C for 3-4 hr, cooled to 15-25 °C, and analyzed by HPLC to determine if pre-set specifications are met, e.g., Intermediate 4 (Stage 10) NMT 1.0%. If this limit is not met, the previous warming and cooling whilst stirring is repeated. Upon HPLC indicating that not more than approximately 1.0% of Intermediate 4 remains, the reaction mixture is cooled to -5 ⁇ 5 °C. Aqueous THF (91%, e.g., 1.09 kg / kg of 10% LAH) is added at NMT 25 °C, and stirring is continued for 20-30 min.
  • Aqueous THF (91%, e.g., 1.09 kg / kg of 10% LAH
  • the water charge (as aqueous THF) may be 1.0-1.1 L of water / kg of LAH, and in a further embodiment may be 1.1 L of water / kg of LAH.
  • Aqueous NaOH (5.3%, e.g., 0.37 kg /kg of 10% LAH) is added at NMT 25 °C (causing an exothermic reaction), and stirring is continued for 20-30 min.
  • the NaOH charge may be 0.17-0.19 mol/mol of LAH , and in a further embodiment may be 0.18-0.19 mol/mol of LAH.
  • the mixture is warmed slowly to 65-70 °C, stirred for 3-4 hr, and cooled to 15-25 °C.
  • the mixture is filtered, using THF (e.g., 30 kg) to complete the transfer of the reaction mixture into the filter.
  • THF e.g., 30 kg
  • the filtrate is kept in the receiver.
  • This filter cake is then transferred back to the reactor and resuspended in fresh THF (1.3 kg / kg of 10% LAH).
  • the mixture is stirred at 15-25 °C for 1-1.5 hr, and then filtered, using THF (0.65 kg / kg of 10% LAH) to complete the transfer again.
  • the wet cake is discarded.
  • the combined filtrates are distilled at ⁇ 100 torr and NMT 40 °C until the batch residue is about 40 L. The distillate is discarded.
  • TBME e.g., 30 kg
  • TBME e.g., 30 kg
  • tap water e.g. 20 kg
  • the aqueous layer is discarded.
  • Tap water e.g., 20 kg
  • the aqueous layer is discarded.
  • the organic layer is analyzed by inductively coupled plasma - optical emission spectroscopy to determine if pre-set specifications are met, e.g., Li NMT 10 ppm, Al NMT 10 ppm. If these specifications are not met, the wash with tap water is repeated until the specifications are met. Following meeting the specifications, anhydrous ethanol (e.g., 30 kg) is added to the organic layer meeting the specifications and the mixture is distilled at ⁇ 100 torr and a pot temperature of NMT40 °C until the batch residue is about 40 L. The distillate is discarded.
  • pre-set specifications e.g., Li NMT 10 ppm, Al NMT 10 ppm. If these specifications are not met, the wash with tap water is repeated until the specifications are met. Following meeting the specifications, anhydrous ethanol (e.g., 30 kg) is added to the organic layer meeting the specifications and the mixture is distilled at ⁇ 100 torr and a pot temperature of NMT40 °C until the batch residue is about 40 L. The distill
  • Anhydrous ethanol (e.g., 82.8 kg) is added to the residue and the mixture is again distilled at ⁇ 100 torr and a pot temperature of NMT 40 °C until the batch residue is about 40 L. The distillate is discarded. This azeotropic distillation step may be repeated one or two more times until pre-set specifications are met, e.g., Karl Fischer moisture analysis indicates a value of NMT 0.5%.
  • the batch residue is then cooled to 15-25 °C and TBME ((tert-butyl methyl ether) e.g., 13.8 kg / kg of Intermediate 4 (Stage 10)) is added to the residue. The mixture is cooled to 0-5 °C.
  • Hydrogen chloride (HC1) gas (3.3 equiv) is added in portions at NMT 25 °C, and stirring is continued for 60-70 min at 20-25 °C after the addition is complete. If the pre-set specification, e.g., pH NMT 1.0, is not met, more HC1 gas is added until the specification is met. The resulting precipitate is collected by centrifugation. The wet cake is washed in the centrifuge cart with TBME:EtOH (anhydrous, 1.5:1.0, e.g., 5.0 kg), and the cake is centrifuged at full speed for 20 ⁇ 5 min.
  • TBME:EtOH anhydrous, 1.5:1.0, e.g., 5.0 kg
  • the cake is analyzed by HPLC to determine if pre-set specifications are met, e.g., Intermediate 5 (Stage 11) NLT 98.0%. If this specification is not met, the cake can be re-suspended in TBME:EtOH (anhydrous, 1.5:1.0, e.g., 6.6 kg / kg of Intermediate 4 (Stage 10)), and centrifuged and washed as above until the specification is met.
  • the cake that meets the specification is dried at NMT 80 torr and 35 ⁇ 5 °C for NLT 12 hr until LOD is NMT 1.0%. Material which does not meet pre-set specifications is dried further at NMT 80 torr and 35 ⁇ 5 °C for NLT 6 hr and re-sampled.
  • tasimelteon which is unmilled, may be synthesized.
  • the end step synthesis of tasimelteon can comprise contacting and reacting ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanaminium chloride (Intermediate 5) with propionyl chloride in the presence of organic solvent and base. Said reaction is illustrated in the following scheme:
  • a first reaction mixture is prepared by adding 45% aqueous NaOH (8 equiv) to a mixture of Intermediate 5 (Stage 11, 1.00 equiv), TBME (e.g., 15.2 kg / kg of Intermediate 5 (Stage 11)) and tap water (e.g., 14.6 kg / kg of Intermediate 5 (Stage 11)) at 0-10 °C.
  • Propionyl chloride (1.28 - 1.46 equiv) is added at 5-10 °C, after which the mixture is stirred at this temperature for 90-120 min.
  • EtOH e.g., 24.0 kg
  • To the pot containing the residue is added 95% EtOH and process water via a filter.
  • the volume of EtOH may be 3.0-5.0 equivalent volumes.
  • the ratio of EtOH:water may be 0.7:1 - 1.4:1 (v/v).
  • the ratio of EtOH:water may be 1.0:1.0.
  • the mixture may be warmed to 35-40 °C and stirred for 30- 40 min, cooled to 13-17°C over a period of 60-120 min, and stirred at 13-17 °C for 60-90 min. If crystallization does not occur, the mixture may be seeded with tasimelteon (unmilled) crystals. Following addition of process water (e.g., 19.2 kg / kg of
  • Material not meeting the preset specifications, e.g., for Impurities 5 and 6 is transferred back to the reaction vessel and recrystallized as described above, i.e., by re-dissolving in warm EtOH:water, filtering, allowing the mixture to cool and crystallize, further precipitating by slow addition of water and collecting by centrifugation.
  • Such re-processed material that meets said impurity specifications is washed, dried and analyzed as described above, after which it is released for milling, discarded, or further re-processed.
  • the above-described end-step synthesis is illustrative only.
  • other organic solvents or mixtures thereof can be used in place of tert-butyl methyl ether (TBME).
  • Bases other than or in addition to NaOH can also be employed.
  • the solvent for crystallization can be an aqueous solvent, such as an aqueous C1-C4 alcohol, e.g., methanol, ethanol, propanol, isopropanol, n-butanol, sec-butanol, isobutanol, or tert- butanol, or a mixture of organic solvents such as MTBE-EtOH-cyclohexane.
  • Tasimelteon drug substance is stored as the unmilled drug substance and milled on an as-needed basis, immediately prior to its use in capsule drug product manufacturing. It has been found that use of a jet mill and a dry nitrogen atmosphere is advantageous in achieving uniform particle size with good handling characteristics and minimal loss.
  • Drug substance meeting particle size specifications e.g., Do.i ⁇ 15 ⁇ (i.e., 10% of the particles are 15 ⁇ in diameter or less); Do.s ⁇ 30 ⁇ ; Do.9 ⁇ 75 ⁇ for in process and (i) a D90 specification set at ⁇ 105 ⁇ ; (ii) a D50 specification set at ⁇ 45 ⁇ ; and (iii) a D10 specification set at ⁇ 15 ⁇ for release) is tightly sealed, e.g., in PE bags and/or aluminum bags, e.g., with a dessicant such as a silica dessicant.
  • a dessicant such as a silica dessicant.
  • tasimelteon When manufacturing pharmaceutical grade tasimelteon, i.e., tasimelteon that is intended for human use, good manufacturing practices (GMP) are employed such as may be required by regulatory bodies in relevant jurisdictions. Bulk pharmaceutical grade tasimelteon is then mixed with excipients to prepare bulk formulated tasimelteon and then formed into an appropriate pharmaceutical dosage form, such as capsules, each comprising 10 mg to 100 mg, e.g., 20 mg, of tasimelteon.
  • GMP good manufacturing practices
  • milling refers to particle size reduction techniques.
  • particle size reduction techniques e.g., sieving, high shear fluid processing, etc.
  • milling techniques other than jet milling e.g., grinding, cryogenic grinding, cutting or impacting, etc., can also be employed.

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Abstract

A process for preparing a batch of highly purified, pharmaceutical grade tasimelteon comprises analyzing a batch of tasimelteon synthesized under GMP conditions for the presence of one or more identified impurities.

Description

HIGHLY PURIFIED PHARMACEUTICAL GRADE TASIMELTEON
Cross-reference to Related Applications
This application claims the benefit of co-pending U.S. Provisional Application Serial No. 61/938,932, filed 12 February 2014, and co-pending U.S. Provisional Application Serial No. 62/087,394, filed 04 December 2014, both of which are hereby incorporated by reference herein.
Field of the Invention
The disclosure relates generally to the synthesis of tasimelteon. In some embodiments, impurities, which may be by-products or degradation products, are analyzed and controlled in order to keep the impurities below pre-set specifications.
Background of the Invention
Tasimelteon, N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)- propionamide, is a melatonin agonist useful in the treatment of persons suffering from certain sleep-related disorders.
A synthesis of tasimelteon is disclosed, e.g., in Example 2 of US 5,856,529. The end step synthesis in that example comprises reaction of ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanamine with propionyl chloride. Synthesis of the methanamine intermediate is described in Preparation 24 and comprises reaction of ((lR,2R)-2-(2,3- dihydrobenzofuran-4-yl))cyclopropanecarboxaldehyde with hydroxylamine
hydrochloride. Synthesis of the carboxaldehyde intermediate is described in
Preparation 18 and comprises palladium catalyzed cyclization of a propenoyl intermediate, specifically, (lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)propenoyl)-2,10- camphorsultam.
Summary of the Invention
In one illustrative embodiment, the invention relates to a process for synthesizing highly purified, pharmaceutical grade tasimelteon, the process comprising: (a) propionylating ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) methanamine or a salt thereof to yield tasimelteon;
(b) crystallizing the tasimelteon produced in step (a);
(c) assaying the crystallized tasimelteon from step (b) for the presence of one or both of Impurity 5 (N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran- 4-yl) cyclopropyl) (propionamido)methyl) cyclopropyl) methyl) propionamide) and Impurity 6 (2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate) ; and
(d) (i) if the crystallized tasimelteon meets pre-set specifications for Impurity 5 or Impurity 6, or both, then collecting the highly purified, pharmaceutical grade tasimelteon or
(d) (ii) if the crystallized tasimelteon fails to meet pre-set specifications for Impurity 5 or Impurity 6, or both, then further purifying the tasimelteon and repeating steps (c) and (d), or discarding the batch.
In another illustrative embodiment, the invention relates to a process for preparing a batch of highly purified, pharmaceutical grade tasimelteon, the process comprising: (a) analyzing a batch of tasimelteon synthesized under conditions of Good
Manufacturing Practices ("GMP conditions") for the presence of an identified
impurity (ies) that is (are) one or more of:
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3- methylbutanamide (Impurity 1),
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide (Impurity 2),
• l,3-Bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea
(Impurity 3),
• N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4)
• N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5) , • 2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6),
• N-(((lR,2R)-2-(3-Oxo-2,3-dihydrobenzofuran-4- yl) cyclopropyl) methyl) propionamide (Impurity 7)
and
(b) if the batch meets pre-set specifications for the amount of the one or more of Impurity 1, Impurity 2, Impurity 3, Impurity 4, Impurity 5, Impurity 6, or Impurity 7, then continuing to process the tasimelteon to prepare bulk tasimelteon drug substance for formulation or
(c) if the tasimelteon does not meet said pre-set specifications, then further purifying (such as by recrystallization, trituration, extraction, or chromatography) the
tasimelteon and repeating steps (a) and (b) or discarding the batch.
In another illustrative embodiments, further specifications for continuing to process the tasimelteon are pre-set, e.g., that the tasimelteon is not less than ("NLT") 95.0%, or NLT 98.0% pure (by area under the curve) and/or that the amount of any other single impurity is NMT 0.10 area%.
In another illustrative embodiment, the invention relates to a process for preparing a batch of tasimelteon drug product (i.e., tasimelteon plus excipients) wherein release of a batch of tasimelteon bulk drug substance for use in the manufacture of the tasimelteon drug product is contingent upon the testing and application of acceptance criteria for the amounts of one or more of the following impurities:
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3- methylbutanamide (Impurity 1),
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide (Impurity 2),
• l,3-Bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea
(Impurity 3),
• N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4) • N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5) ,
• 2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6),
• N-(((lR,2R)-2-(3-Oxo-2,3-dihydrobenzofuran-4- yl) cyclopropyl) methyl) propionamide (Impurity 7).
In a further illustrative embodiment, the invention relates to purified tasimelteon wherein the tasimelteon does not contain any of Impurities 1 through 7 at a
concentration greater than about 0.15%. In related illustrative embodiments, such composition does not contain any related-substance impurity (i.e., an impurity that is structurally related to tasimelteon such as degradation products, dimers, etc.) at a concentration of greater than about 0.15% by weight.
Detailed Description of the Invention
The synthesis of tasimelteon can result in a plurality of impurities following the end step synthesis. An illustrative synthesis of tasimelteon is a linear process, passing through a methanamine intermediate such as by the process described in US 5,856,529 and involving four purification steps: one purification step for each of three isolated intermediates, as described below, as well as one for the unmilled tasimelteon drug substance. (lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropanecarboxylate (herein referred to as Intermediate 3 or Stage 9), (lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropane carboxamide (herein referred to as Intermediate 4 or Stage 10), and the methanamine intermediate (herein referred to as Intermediate 5 or Stage 11) and the tasimelteon (unmilled) drug substance are each isolated by crystallization and, if necessary, are subjected to recrystallization to improve purity.
The inventors have discovered that in the synthesis of tasimelteon there are certain impurities that can be formed as both by-products and degradation products, and that these impurities can be controlled or reduced to non-detectable or acceptably detectable levels. Although not desiring to be bound by theory, the inventors have identified some of these impurities on the basis of mass spectrometric, nuclear magnetic resonance spectroscopic and other data. The inventors have found that the impurities can include one or more of:
N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3-methylbutanamide (Impurity 1),
N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide
(Impurity 2),
l,3-bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea (Impurity 3), N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4), N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5), 2 - hydro xy-6- (2 - (propionamidomethyl) cyclopropyl) phenethyl 2- (2 -hydroxy ethyl) - 3 - (2 - (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6), and
N-(((lR,2R)-2-(3-oxo-2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 7).
Impurities 1-3 and 5-6 may be by-products of certain steps of the synthesis of tasimelteon, and impurities 4 and 7 may be degradation products.
The inventors have also found that in the synthesis of tasimelteon, there are certain additional impurities that can occur as degradation products, reaction byproducts, residual reagents, and residual intermediates. These additional impurities can be controlled or reduced to non-detectable or acceptably detectable levels. These impurities can include (+)-dehydroabietylamine, propionyl chloride, propionic acid, ethyl propionate [possibly additional potential degradants of propionyl chloride], ethyl diazoacetate, Intermediates 2, 4, and 5, 4-vinyl-2,3-dihydrobenzofuran (VBF), 4-(2- chloroethyl)-2,3-dihydrobenzofuran (VBF-int-2), benzene, and heavy metals such as As, Al, Fe, Li, Ni, Ru, Pd, Mn, Rh, Cu, and Co.
Some such impurities, such as ethyl diazaoacetate and propionyl chloride, are
potentially genotoxic and must be controlled to ppm levels in order for the bulk GMP tasimelteon to be suitable for formulation into bulk pharmaceutical composition and subsequently distributed into pharmaceutical dosage units. The identification of such impurities facilitates quality control and consistency of product. With the knowledge of the identities of these impurities, a manufacturer of tasimelteon can set specifications for the maximum allowable amount of the impurities in bulk GMP tasimelteon, which can then be formulated into bulk pharmaceutical composition and then distributed into pharmaceutical dosage units.
Thus, in one aspect, this invention comprises a batch of pharmaceutical grade, highly purified tasimelteon that has been analyzed for the presence of any or each of these impurities and determined to have less than a pre-determined amount of one or more of them. The pre-determined amounts, i.e., the pre-set specifications, for these
intermediates can be set to satisfy regulatory requirements. For example, the pre-set specification for Impurities 1-7 and the additional impurities can be 0.15 wt%. In a further embodiment, the pre-set specification can be 0.10 area%, e.g., for unidentified impurities. Additionally, a pre-set specification may include not more than (NMT) lOOppm or NMT 10 ppm of ethyl diazaoacetate (EDA)
The impurities are detectable by analytical chemical techniques such as
chromatographic and mass spectrometry techniques among others. For example, HPLC, GC, or other chromatography methods can be used, in which case the amount of one or of each of the impurities can be determined on the basis of wt% or of area under the curve.
As used herein, abbreviations for methods and techniques may include: High- performance Liquid Chromatography (HPLC), Ultra Performance Liquid
Chromatography (UPLC), Supercritical fluid chromatography (SFC), Gas
chromatography (GC), Good Manufacturing Practices (GMP), Current Good
Manufacturing Practices (cGMP), not more than (NMT), and not less than (NLT).
References herein to percent (%) purity are based on area. Such relative quantities approximate weight % but persons skilled in the art know how to determine more precise weight % amounts if desired. A synthesis of tasimelteon is disclosed, e.g., in Example 2 of US 5,856,529. The end step synthesis in that example comprises reaction of ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) methanamine with propionyl chloride. Synthesis of the methanamine intermediate is described in Preparation 24 and comprises reaction of ((lR,2R)-2-(2,3- dihydrobenzofuran-4-yl))cyclopropanecarboxaldehyde with hydroxylamine
hydrochloride. Synthesis of the carboxaldehyde intermediate is described in
Preparation 18 and comprises palladium catalyzed cyclization of a propenoyl intermediate, specifically, ((lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)propenoyl)-2,10- camphorsultam.
An alternative route to the methanamine intermediate or a salt thereof (herein referred to as Intermediate 5) proceeds through (lR,2R)-2-(2,3-dihydrobenzofuran-4- yfjcyclopropanecarboxylate (Intermediate 3) to (lR,2R)-2-(2,3-dihydrobenzofuran-4- yfjcyclopropane-carboxamide (Intermediate 4) and then to Intermediate 5 or a salt thereof.
A synthesis of Intermediate 2 by stereoselective cyclization of 4-vinyl-2,3- dihydrobenzofuran is described, e.g., in US 7,754,902.
An illustrative end-step synthesis of tasimelteon from Intermediate 5 is provided in Scheme 6, below. In general, the synthesis comprises:
(a) propionylating ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) methanamine or a salt thereof to yield tasimelteon;
(b) crystallizing the tasimelteon produced in step (a);
(c) assaying the crystallized tasimelteon from step (b) for the presence of one or both of Impurity 5 (N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran- 4-yl) cyclopropyl) (propionamido)methyl) cyclopropyl) methyl) propionamide) and Impurity 6 (2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate) ; and (d) (i) if the crystallized tasimelteon meets pre-set specifications for Impurity 5 or Impurity 6, or both, then collecting the highly purified, pharmaceutical grade tasimelteon or
(d) (ii) if the crystallized tasimelteon fails to meet pre-set specifications for Impurity 5 or Impurity 6, or both, then further purifying the tasimelteon and repeating steps (c) and (d), or discarding the batch.
In such end-step synthesis, the propionylating step may comprise contacting ((1R,2R)- 2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methanamine or a salt thereof with a propionyl halide, a propionyl anhydride, a propionyl ester, a propionyl amide, a propionyl imidazolide, or with propionic acid and a dehydrating agent or the product thereof. Water is a byproduct of the coupling of ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanamine with propionic acid to form tasimelteon. The dehydrating agent, which is also known as a peptide coupling reagent, is an agent that activates propionic acid toward reaction with ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanamine and consumes the byproduct, water. Commonly used dehydrating agents include but are not limited to dicyclohexylcarbodiimide (DCC), DCC and an aminopyridine, Ν,Ν'-carbonyldiimidazole, chlorosilanes, Amberlyst-15,
MeS02Cl-Et3N, BF3, TiC14, other Lewis acids, reagents of the type ArB(OH)2,
Sn[N(TMS)2], POC , molecular sieves, Lawesson's reagent, and (MeO)2POCl.
The propionylation may be carried out in the presence of an organic solvent (e.g., ter- butyl methyl ether) and an aqueous base (e.g., NaOH), After the propionylation step and before the crystallizing step, the mixture of tasimelteon may be assayed for the presence of Intermediate 5 (or the free base or other salt thereof) and, if the mixture does not meet pre-set specifications for Intermediate 5 (e.g., not more than 0.15 % or not more than 0.10 %), then repeating step (a) or discarding the mixture. After the propionylation step and before the crystallizing step, the mixture of tasimelteon may be washed with aqueous base and the aqueous layer discarded, after which the washed mixture may be distilled (e.g., in ethanol at up to about 58 °C, and less than about 100 mmHg). The crystallization step may comprise dissolving the tasimelteon by stirring and warming a mixture of the tasimelteon and a C1-C4 alkanol (e.g., about 35 to about 40 °C) and then cooling (e.g., to about 13 to about 17 °C) while stirring. The crystallization step optionally comprises seeding.
An illustrative synthesis of tasimelteon, in one embodiment, can include the following reaction schemes with a number of intermediates being synthesized first.
Synthesis of 4-(2-Chloroethyl)-2.3-dihydrobenzofuran (VBF-int-2)
The synthesis of VBF-int-2 can comprise contacting and reacting 2,3-Bis(2- hydroxyethyl) phenol (Triol) with N,N-dimethylchloromethyleneiminium chloride (the Vilsmeier reagent) in an organic solvent, followed by reacting the resulting N,N'-[(3- hydroxy-l,2-phenylene)-bis(ethane-2,l-diyloxymethylidene)] -bis(N- methylmethanaminium) dichloride (VBF-int-1) with triethylamine in an organic solvent. The Vilsmeier reagent may be generated in situ from N,N-dimethylformamide (DMF) and oxalyl chloride. Said reaction is illustrated in the following scheme:
Figure imgf000010_0001
VBF-int-1 (Stage 4) VBF-int-2 (Stage 5)
[Scheme 1]
For example, a first reaction mixture can be prepared by slowly adding oxalyl chloride (approximately 2.45-2.55 equiv) to a solution of DMF (approximately 2.45-2.55 equiv) in CH3CN (Acetonitrile (e.g., 16% by weight DMF)) at -10±5 °C while maintaining the batch temperature at -10±5 °C. Stirring may be continued at this temperature for approximately 30-40 min to complete the formation of the Vilsmeier reagent
(N,Ndimethylchloromethyleneiminium chloride) in situ. Triol (Stage 3) (1.00 equiv; e.g., 30 kg) is added to the solution of the Vilsmeier reagent in portions through an addition funnel while maintaining the batch temperature at -10±5 °C. Stirring is continued at about -20 to about -5 °C for at least 90 min, until testing via high pressure liquid chromatography (HPLC) indicates that no more than (NMT) 2.0% Triol (Stage 3) remains in solution. If necessary, the mixture can be sampled again at 150 min and tested again for Triol levels. Following this, a solution of Et3N (triethylamine
(approximately 3.8-4.1 equfvj) in CH3CN (e.g., 47% by weight Et3N) may be slowly added to the reaction mixture while maintaining the batch temperature at -10 ±5 °C. This step is an exothermic step. The total volume of CH3CN should be approximately 5- 17 L/kg of Triol (Stage 3) input, and in one embodiment may belO L/kg of Triol (Stage 3) input. When the addition is complete, the mixture may be heated to 55±5 °C for 3-3.5 hr. The mixture may then be cooled to 25±5 °C and stirred for up to four increments of up to approximately 1 hr each until HPLC indicates VBF-int-1 (Stage 4) NMT 2.0 area%. Tap water (e.g., 2.3 L / kg of Triol (Stage 3)) is then added to this reaction mixture, and stirring is continued for 30-40 min. The mixture is distilled at <100 torr and less than approximately 40 °C until no more organic distillate is collected. TBME (e.g., 5.6 kg / kg of triol (Stage 3)) and tap water (e.g., 3.2 L / kg of Triol (Stage 3)) are then added to the batch residue. The mixture is stirred for 30-40 min and settled for 30-40 min. The aqueous layer is removed. A solution of H3PO4 (8.5% by weight) in aqueous brine (e.g., 5 kg of H3PO4 solution / kg of Triol (Stage 3)) is slowly added to the remaining organic layer. This mixture can be stirred for 30-40 min and settled for 30-40 min. The aqueous layer is removed once more. The organic phase can be washed one or more times with tap water (e.g., 5 L / kg of Triol (Stage 3)) , each time stirring for approximately 30-40 minutes, settling for approximately 30-40 min, and removing the aqueous layer.
Following the washing with tap water, the organic layer is distilled at <100 torr and less than approximately 40 °C until no more distillate is collected. The batch residue is subjected to short path distillation at 0.1 - 4 torr. Any distillate boiling below 105°C is discarded. The distillate boiling at 105-130 °C is subjected to HPLC analysis. Material meeting a pre-set specification, e.g., VBF-int-2 (Stage 5) present at not less than (NLT) 95.0%, is used directly in the next step.
Synthesis of 4-Vinyl-2,3-dihydrobenzofuran (VBF) (Stage 6)
The synthesis of VBF can comprise contacting and reacting 4-(2-Chloroethyl)-2,3- dihydrobenzofuran (VBF-int-2) with tetrabutylammonium hydroxide in the presence of organic solvent. Said reaction is illustrated in the following scheme: VB
Figure imgf000012_0001
F-int-2 (Stage 5) 6)
[Scheme 2]
In one embodiment, tetrabutylammonium hydroxide (0.78 kg / kg of VBF-int-2 (Stage 5)), potassium iodide (0.09 kg / kg of VBF-int-2 (Stage 5)) and VBF-int-2 (from above (Stage 5)) is added to a mixture of TBME (tert-Butyl methyl ether) (5.60 kg / kg of VBFint-2 (Stage 5)) and 45% aqueous NaOH (4.80 kg / kg of VBF-int-2 (Stage 5)). In some embodiments, the NaOH, tetrabutylammonium hydroxide and KI charges are in the ranges 7-10, 0.15-0.50 and 0.08-0.10 molar equivalents, respectively. The mixture may be heated to 50±5 °C and stirred for approximately 3-3.5 hr. The mixture is then cooled to 25±5 °C and stirred for up to four increments of NLT 1 hr each until testing via HPLC indicates VBF-int-2 Stage 5) NMT 1.0%. The mixture is settled for 20-30 min and 40-60 L of the aqueous layer is discharged. 16% aqueous HC1 (e.g., up to 6.2 kg / kg of VBFint-2 (Stage 5)) is added slowly to the remaining mixture until the pH of the mixture is 9.5 - 10.5. If necessary, 4.5% aqueous NaOH is added to adjust the pH into this range. The mixture can then be filtered using TBME (1 kg / kg of VBF-int-2 (Stage 5)) to complete the transfer and the filtrate settled for 20-30 minutes. The aqueous layer may then be removed. 8% Na2S203 in 9% aqueous brine (e.g., 4.3 kg of Na2S203 solution / kg of VBF-int-2 (Stage 5)) is added to the organic layer, then the mixture is stirred for 10- 15 min and settled for 20-30 min and the aqueous layer is removed. To the organic layer is added 4% NaOH in 9% aqueous brine (e.g., 4.2 kg of NaOH solution / kg of VBF-int-2 (Stage 5)) followed by stirring, settling and removal of the aqueous layer. Then quinol (e.g., 7 g / kg of VBF-int-2 (Stage 5), or 1 mol%) is added to the organic layer and the mixture is stirred for 20-30 min. The resulting solution is subjected to HPLC analysis for purity and assay. Material meeting pre-set purity specification, e.g., VBF (Stage 6) NLT 95.0 area%, is used directly in the next step. The assay result from HPLC is reported as %wt/wt. Synthesis of (lj?,2j?)-2-(2,3-Dihydrobenzofuran-4-yl) (Intermediate 3) (Stage 9)
The synthesis of Intermediate 3 (Stage 9) can comprise asymmetric cyclopropanation of 4-vinyl-2,3-dihydrobenzofuran (VBF (Stage 6)) by contacting and reacting it with EDA in the presence of a chiral catalyst. It can also comprise hydrolysis of the ester group of 2-(2,3-dihydrobenzofuran-4-yl)-cyclopropanecarboxylic acid ethyl ester (VEC-int-1 (Stage 7)) followed by polishing resolution of 2-(2,3-dihydrobenzofuran-4-yl)- cyclopropanecarboxylic acid (Intermediate 2 (Stage 8)) with (+)-dehydroabietylamine (DAA) in an organic solvent. Said reaction sequence is illustrated in the following scheme:
Figure imgf000013_0001
Figure imgf000013_0002
[Scheme 3]
In one embodiment, in order to form Intermediate 3, a number of processes may be utilized in preparation.
A lithium diisopropylamide (LDA) solution may be prepared. For instance, a solution of n-butyllithium (0.03 equiv; 1 M in hexanes) is added, slowly, to a solution of
diisopropylamine (DISPA; 0.04 equiv; e.g., 10 M) in THF at 5±5 °C. After the addition iscomplete, stirring is continued at 5±5 °C for 30-40 min. The resulting solution of lithium diisopropylamide (LDA) is used directly for the subsequent deprotonation of BTBSC ((i?,i?)-(-)-N,N'-Bis(3,5-di-ter^utylsalicylidene)-l,2 cyclohexanediamine), as further described below.
A Ru catalyst may be prepared from BTBSC and the LDA solution. For instance, the preparation can comprise stirring a mixture of BTBSC (0.02 equiv; e.g., 0.04 M) in THF (tetrahydrofuran) at 25±5 °C for 30-40 min, and then cooling the mixture to 5±5 °C. The LDA solution from above may then be added slowly to this mixture at 5±5 °C and the mixture stirred for approximately 60 min. To the resulting mixture is added, in portions, [Ru(pcymene)Ch]2 (0.02 equiv, assuming 2 equiv Ru / mole of [Ru(p-cymene)Ch]2) . The reactor is purged three times with N2. The mixture is stirred at 25±5 °C for 30-40 min. Lastly, VBF (Stage 6) solution (ca. 0.01 equiv) in TBME is added to this mixture. The resulting mixture is stirred at 20-25 °C for at least approximately 8 hours. The resulting Ru catalyst mixture is used directly in the subsequent cyclopropanation of VBF step.
VBF (Stage 6) may undergo cyclopropanation. For instance, in one embodiment, such a preparation may comprise adding toluene (e.g., 20 kg) to the VBF (Stage 6) solution (1.00 equiv) prepared as described for the preceding step in TBME (e.g., weight of solution (kg) = 8.9 / assay%) and distilling the mixture at <100 torr and < 50°C until about 20 L of residue remains in the reaction vessel. Toluene (e.g., 60 L) is added, and the mixture is again distilled at <100 torr and < 50°C until about 20 L of residue remains in the reaction vessel. The batch residue is cooled to 30±2 °C, and the Ru catalyst prepared above is added. The Ru catalyst charge can include an amount of
approximately 0.02 molar equivalents. To this mixture is added a solution of EDA in toluene over 8-16 hr at 30±2 °C. The ethyl diazoacetate charge can include
approximately 2.5 molar equivalents. The mixture is stirred for at least approximately 3 hr at 30±2 °C after the addition is complete. Material for which UPLC analysis shows NMT approximately 2.0% VBF (Stage 6) is used directly in the next preparation step, described in further detail below.
VEC-int-1 (Stage 7) may undergo a saponification. An illustrative example may include adding 45% aqueous NaOH (4 equiv), 55% aqueous tetrabutylammonium hydroxide (TBAH; 0.45 equiv) and tap water (e.g., 10 L) to the final reaction mixture from the cyclopropanation of VBF. This mixture is then stirred at 50-70 °C for 16-18 hr until HPLC indicates <2.0% VEC-int-1 (Stage 7). If the limit is not met, stirring is continued at 50-70 °C for 2-4 hr and the analysis is repeated. Once the limit is met, the mixture is cooled to 25-30 °C. Tap water (e.g., 60.0 L) is added and the mixture is stirred for at least approximately 30 min, and settled for 30-40 min. The organic layer is discarded. TBME (e.g., 107.0 kg) is added to the resulting aqueous layer and the mixture is cooled to 0-10 °C. Phosphoric acid (85% aqueous, e.g., 24.0 kg) is added slowly at 0-25 °C until the pH of the aqueous layer is 4.0-4.5. If necessary, 10% aqueous NaOH is added to bring the pH into this range. The mixture is then stirred for at least approximately 30 min and settled for another 30-40 min, the aqueous layer being discarded. Tap water (e.g., 70.0L) is added and the mixture is stirred for at least approximately 30 min and settled again for approximately 30-40 min, and the aqueous layer is discarded. This tap water wash may be repeated, for instance three more washes may be utilized.
Lastly, the Intermediate 3 (Stage 9) (DAA salt) may be formed. In an illustrative example, TBME (e.g., 22.9 kg / kg of VBF (Stage 6)) and ethanol (EtOH; anhydrous, e.g., 4.49 kg / kg of VBF (Stage 6) may be added to the resulting organic layer from the saponification preparation step above. The ratio of Intermediate 2 (Stage 8) to TBME may be included in a range of 0.040-0.079 kg Intermediate 2 (Stage 8) / L TBME, and in a further embodiment may comprise a set point of 0.040 kg Intermediate 2 (Stage 8) / L TBME. In one embodiment, the ratio of TBME (kg):EtOH (kg) may be 7.78-9.08, and in a further embodiment may be 7.78. Next, (+)-dehydroabietylamine (1.44 equiv) as a 28% wt/wt solution in TBME may be added to the resulting mixture. In one embodiment, the (+)-dehydroabietylamine charge may be 1.44-1.76 molar equivalents, and in a further embodiment may be 1.44 molar equivalents. This reaction mixture may be heated to 45- 55 °C and stirred for NLT 20 min, cooled to 25-30 °C in a period of NLT 2 hr and stirred at this temperature for NLT 1 hr, heated to 45-55 °C and stirred for NLT 20 min, cooled to 15-25 °C in a period of NLT 2 hr and stirred for NLT 4 hr, cooled to 0-5 °C in a period of NLT 1 hr and stirred for NLT 1 hr, and the precipitated solid is collected by
centrifugation, washed with TBME, and spun, e.g., at full speed for 20±5 min. The collected wet cake is added to ethanol (anhydrous, e.g., 11.2 kg / kg of VBF (Stage 6)) that has been cooled to 0-5 °C. The mixture is stirred at this temperature for 30-40 min and then centrifuged, e.g., at full speed for 20±5 min. This washed wet cake is subjected to purity analysis by HPLC. Material meeting pre-set specifications, e.g., R,R)-trans- Intermediate 3 (Stage 9) NLT 99.0 area% and total impurities NMT 2.0%, is dried at NMT 80 torr and 60±5 °C for NLT 12 hr until loss on drying (LOD) meets a pre-set specification e.g., LOD NMT 2.0%. Material failing this specification is dried further at NMT 80 torr and 60±5 °C for NLT 6 hr and re-sampled.
Material meeting the specification is released. If the wet cake fails the purity test, it is processed again. The second process may comprise adding the wet cake to a cooled (e.g., 0-10 °C) mixture of 45% aqueous NaOH (e.g., 3.60 kg/kg of VBF (Stage 6)), tap water (e.g., 11.9 kg/kg of VBF (Stage 6)) and toluene (e.g., 4.49 kg/kg of VBF (Stage 6)), stirring for about 30 min, settling for about 30 min, and phase separation. To the aqueous layer is added TBME (e.g., 12.0 kg/kg of VBF (Stage 6)) and the mixture is cooled (e.g., to 0-10 °C). The pH of the aqueous layer is adjusted with phosphoric acid (85% aqueous, e.g., 24.0 kg) and, if necessary, 10% aqueous NaOH to a value of 4.0-4.5. After thorough mixing and settling, the layers are separated, and the organic phase is washed several times with tap water. Formation, isolation, drying and LOD and purity analysis of the Intermediate 3 (Stage 9) DAA salt is repeated as described above.
Material meeting the specification is released.
Synthesis of (li?.2i?)-2-(2.3-dihydrobenzofuran-4- yljcyclopropanecarboxamide (Intermediate 4) (Stage 10)
The synthesis of Intermediate 4 can comprise liberation of the free carboxylic acid from (li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl) cyclopropanecarboxylic acid (+)- dehydroabietylamine salt (Intermediate 3) followed by conversion via the
corresponding acid chloride to the amide, (li?,2i?)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropane-carboxamide (Intermediate 4 (Stage 10)). Said reaction sequence is illustrated in the following scheme:
Figure imgf000016_0001
4. Ammonium hydroxide, H20,
heptane
Intermediate 3 Intermediate 4 (+)-Dehydroabietylamine
(Stage 9) (Stage 10) (DAA)
[Scheme 4] In an illustrative example, Intermediate 4 may be synthesized by adding Intermediate 3 (Stage 9) (1 equiv, e.g., 20.0-21.0 kg) to a first reaction mixture of tap water (e.g., 5.2 L / kg of Intermediate 3 (Stage 9)), 45% aqueous NaOH (4 equiv), and toluene (e.g., 1.8 kg / kg of Intermediate 3 (Stage 9)) at 20-30 °C. The mixture is then stirred at 25-30 °C for NLT 30 min and settled for 30-40 min, and the organic layer discarded. Toluene (e.g., 1.8 kg / kg of Intermediate 3 (Stage 9)) is added to the aqueous layer, followed by stirring for NLT 60 min, settling for 30-40 min and discarding the organic layer. The toluene wash can be repeated. Next, sodium chloride (e.g., 0.3 kg / kg of Intermediate 3 (Stage 9)) is added to the remaining aqueous layer. The temperature is adjusted to 15-20 °C. Butyl acetate (e.g., 1.2 kg / kg of Intermediate 3 (Stage 9)) is added. Hydrochloric acid (32% aqueous, 2.9 equiv) is added slowly. The temperature is maintained at 15-20 °C while the mixture is stirred for NLT 60 min and settled for 30-40 min. If the pH of the aqueous layer is more than 3, additional 32% HC1 is added until the pH is less than 3. The layers are separated, and the organic layer is set aside for later use. The aqueous layer is added to butyl acetate (e.g., 1.1 kg / kg of Intermediate 3 (Stage 9)). The temperature is maintained at 15-20 °C while the mixture is stirred for NLT 60 min and settled for 30-40 min. The aqueous layer is discarded. The organic layers are combined and distilled at < 100 torr and a pot temperature of NMT 82 °C until the batch residue is about 30 L. The distillate is discarded. Butyl acetate (e.g., 0.71 kg / kg of Intermediate 3 (Stage 9)) is added to the batch residue. This mixture is distilled at < 100 torr and a pot temperature of NMT 82 °C until the batch residue is about 30 L. The distillate is discarded. This step is repeated one or two more times until Karl Fischer moisture analysis indicates a value of less than approximately 0.1%. The batch residue is cooled to 15-20 °C. DMF (0.03 equiv) and thionyl chloride (1.3 equiv) are added. The mixture is heated to 50-55 °C, stirred for 1.5-2.0 hr and cooled to 21±4 °C, and analyzed by HPLC. Material meeting pre-set specifications, e.g., Intermediate 2 (Stage 8) NMT 1.0%, is further processed. If this specification is not met, additional thionyl chloride (0.12 equiv) is added, and the mixture is heated to 50-55 °C, stirred for 1.5-2.0 hr, cooled to 21±4 °C, and re-sampled. Following this, a mixture of ammonium hydroxide (9.0 equiv) and tap water (e.g., 0.8 L / kg of Intermediate 3 (Stage 9)) is cooled to 0-5 °C. The acid chloride solution from the previous step meeting the pre-set specification is added in portions while maintaining the batch temperature at 0-10 °C. After the addition, stirring is continued for 30-40 min at 0-10 °C. Then n-Heptane (e.g., 1.3 kg / kg of Intermediate 3 (Stage 9)) is added, and stirring is continued for 2-3 hr at 0-10 °C. The resulting precipitate is collected by centrifugation. The wet cake is washed in the centrifuge cart with tap water (e.g., 15 L / cart) and then spun at full speed for 20±5 min. This wet cake is added to a mixture of butyl acetate (e.g., 0.71 kg / kg of Intermediate 3 (Stage 9)) and n-heptane (e.g., 0.3 kg / kg of Intermediate 3 (Stage 9)) at 0-10 °C. The resulting mixture is stirred for 30-40 min at 0-10 °C and then centrifuged at full speed for 20±5 min. The wet cake is analyzed by HPLC to determine if pre-set specifications are met, e.g., Intermediate 4 (Stage 10) NLT 98.0%. If this specification is not met, the wet cake can be added to another mixture of butyl acetate and n-heptane, the stirring and
centrifugation repeated until the wet cake meets the specification as analyzed by HPLC, e.g., Intermediate 4 (Stage 10) NLT 98.0%. The wet cake that meets the pre-set specifications is dried at NMT 80 torr and 45±5 °C for NLT 12 hr until pre-set specifications are met, e.g., LOD is NMT 1.0% and moisture by Karl Fischer analysis is NMT 0.2%. Material failing these pre-set specifications is dried further at NMT 80 torr and 45±5 °C for NLT 6 hr and resampled. Material meeting the pre-set specifications is released as Intermediate 4 (Stage 10), which may be stored in one or more polyethylene (PE) bags, which may also be sealed within a paper drum.
Synthesis of ((li?.2i?)-2-(2.3-dihydrobenzofuran-4- yl)cyclopropyl)methanaminium chloride (Intermediate 5)
The synthesis of Intermediate 5 can comprise contacting and reacting (li?,2i?)-2-(2,3- dihydrobenzofuran-4- yl)cyclopropanecarboxamide (Intermediate 4) with Lithium aluminum hydride in an organic solvent, followed by aqueous workup and isolation of the resulting amine as its hydrochloride salt. Said reaction is illustrated in the following scheme:
Figure imgf000018_0001
Intermediate 4 Intermediate 5
(Stage 10) (Stage 11)
[Scheme 5] In one example, Intermediate 5 (Stage 11) may be synthesized by the above scheme, wherein the synthesis may include the following procedure. For example, a reactor (e.g., SS316) is cleaned with refluxing acetone (e.g., 100 kg), drained, dried under vacuum for 1-2 hr, and filled with N2 gas. The Intermediate 4 (Stage 10) (1.00 equiv) made above and THF (e.g., 8 kg / kg of Intermediate 4 (Stage 10)) are added to the dry reactor and cooled to -10 °C. Lithium aluminum hydride (LAH) solution (10% in THF, 3.5 - 3.8 equiv, where 1 equiv = 1 mol / mol of Intermediate 4 (Stage 10)) is added in portions while keeping the batch temperature NMT 25 °C. The LAH feed line is rinsed with THF (e.g., 10 kg). The mixture is warmed to 20-30 °C and stirred for 20-30 min. The mixture is then warmed slowly to 65-70 °C while maintaining an internal pressure of NMT 0.1 kg/cm2. This mixture is stirred at 65-70 °C for 3-4 hr, cooled to 15-25 °C, and analyzed by HPLC to determine if pre-set specifications are met, e.g., Intermediate 4 (Stage 10) NMT 1.0%. If this limit is not met, the previous warming and cooling whilst stirring is repeated. Upon HPLC indicating that not more than approximately 1.0% of Intermediate 4 remains, the reaction mixture is cooled to -5~5 °C. Aqueous THF (91%, e.g., 1.09 kg / kg of 10% LAH) is added at NMT 25 °C, and stirring is continued for 20-30 min. The water charge (as aqueous THF) may be 1.0-1.1 L of water / kg of LAH, and in a further embodiment may be 1.1 L of water / kg of LAH. Aqueous NaOH (5.3%, e.g., 0.37 kg /kg of 10% LAH) is added at NMT 25 °C (causing an exothermic reaction), and stirring is continued for 20-30 min. The NaOH charge may be 0.17-0.19 mol/mol of LAH , and in a further embodiment may be 0.18-0.19 mol/mol of LAH. The mixture is warmed slowly to 65-70 °C, stirred for 3-4 hr, and cooled to 15-25 °C. The mixture is filtered, using THF (e.g., 30 kg) to complete the transfer of the reaction mixture into the filter. The filtrate is kept in the receiver. This filter cake is then transferred back to the reactor and resuspended in fresh THF (1.3 kg / kg of 10% LAH). The mixture is stirred at 15-25 °C for 1-1.5 hr, and then filtered, using THF (0.65 kg / kg of 10% LAH) to complete the transfer again. The wet cake is discarded. The combined filtrates are distilled at <100 torr and NMT 40 °C until the batch residue is about 40 L. The distillate is discarded. TBME (e.g., 30 kg) is added to the remaining batch residue and the mixture is distilled at <100 torr and NMT 40 °C until the batch residue is about 40 L. The distillate is discarded. TBME (e.g., 20 kg) and tap water (e.g., 20 kg) are then added to the batch residue and the mixture is stirred for 60-70 min at 15-20 °C and settled for 30-40 min. The aqueous layer is discarded. Tap water (e.g., 20 kg) is then added to the organic layer and the mixture is stirred for 60-70 min at 15-20 °C and settled for 30-40 min. The aqueous layer is discarded. The organic layer is analyzed by inductively coupled plasma - optical emission spectroscopy to determine if pre-set specifications are met, e.g., Li NMT 10 ppm, Al NMT 10 ppm. If these specifications are not met, the wash with tap water is repeated until the specifications are met. Following meeting the specifications, anhydrous ethanol (e.g., 30 kg) is added to the organic layer meeting the specifications and the mixture is distilled at < 100 torr and a pot temperature of NMT40 °C until the batch residue is about 40 L. The distillate is discarded. Anhydrous ethanol (e.g., 82.8 kg) is added to the residue and the mixture is again distilled at < 100 torr and a pot temperature of NMT 40 °C until the batch residue is about 40 L. The distillate is discarded. This azeotropic distillation step may be repeated one or two more times until pre-set specifications are met, e.g., Karl Fischer moisture analysis indicates a value of NMT 0.5%. The batch residue is then cooled to 15-25 °C and TBME ((tert-butyl methyl ether) e.g., 13.8 kg / kg of Intermediate 4 (Stage 10)) is added to the residue. The mixture is cooled to 0-5 °C. Hydrogen chloride (HC1) gas (3.3 equiv) is added in portions at NMT 25 °C, and stirring is continued for 60-70 min at 20-25 °C after the addition is complete. If the pre-set specification, e.g., pH NMT 1.0, is not met, more HC1 gas is added until the specification is met. The resulting precipitate is collected by centrifugation. The wet cake is washed in the centrifuge cart with TBME:EtOH (anhydrous, 1.5:1.0, e.g., 5.0 kg), and the cake is centrifuged at full speed for 20±5 min. The cake is analyzed by HPLC to determine if pre-set specifications are met, e.g., Intermediate 5 (Stage 11) NLT 98.0%. If this specification is not met, the cake can be re-suspended in TBME:EtOH (anhydrous, 1.5:1.0, e.g., 6.6 kg / kg of Intermediate 4 (Stage 10)), and centrifuged and washed as above until the specification is met. The cake that meets the specification is dried at NMT 80 torr and 35±5 °C for NLT 12 hr until LOD is NMT 1.0%. Material which does not meet pre-set specifications is dried further at NMT 80 torr and 35±5 °C for NLT 6 hr and re-sampled. Material meeting the pre-set specifications is released as Intermediate 5 (Stage 11). The resulting Intermediate 5 (Stage 11) may be stored in one or more PE bags, which may in turn be sealed in a paper drum. Synthesis of N-(((lj?,2j?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)- methyl)propionamide (tasimelteon, pre-particle size reduction (i.e., unmilled))
Following the synthesis of the above disclosed intermediates, tasimelteon, which is unmilled, may be synthesized. The end step synthesis of tasimelteon can comprise contacting and reacting ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanaminium chloride (Intermediate 5) with propionyl chloride in the presence of organic solvent and base. Said reaction is illustrated in the following scheme:
Figure imgf000021_0001
Intermediate 5 Tasimelteon (Unmilled)
(Stage 11)
[Scheme 6]
For example, in an illustrative end step synthesis, a first reaction mixture is prepared by adding 45% aqueous NaOH (8 equiv) to a mixture of Intermediate 5 (Stage 11, 1.00 equiv), TBME (e.g., 15.2 kg / kg of Intermediate 5 (Stage 11)) and tap water (e.g., 14.6 kg / kg of Intermediate 5 (Stage 11)) at 0-10 °C. Propionyl chloride (1.28 - 1.46 equiv) is added at 5-10 °C, after which the mixture is stirred at this temperature for 90-120 min. This mixture can be analyzed by HPLC to determine if the resultant solution meets preset specifications, e.g., Intermediate 5 (Stage 11) NMT 0.10%. After stirring and then settling, at 25-30 C, the aqueous layer is discarded. The organic layer can be washed with 5% aqueous NaOH and then twice with water. The organic layer is filtered and distilled at about <100 Torr (1 Torr ~= 1 mmHg = 133.3 Pa) and about </= 58 °C and the distillate is discarded. Into the pot containing this residue is charged 95% EtOH (e.g., 24.0 kg) via a clean filter. The resulting mixture is distilled at about <100 Torr and about </= 58 °C, the distillate is discarded, and this solvent exchange step is repeated two more times with fresh 95% EtOH. To the pot containing the residue is added 95% EtOH and process water via a filter. The volume of EtOH may be 2.8-5.0 equivalent volumes, where 1 equivalent volume = 1 L of EtOH/kg of tasimelteon (unmilled), assuming 90% yield of tasimelteon (unmilled) based on Intermediate 5 (Stage 11) input. In another embodiment, the volume of EtOH may be 3.0-5.0 equivalent volumes. The ratio of EtOH:water may be 0.7:1 - 1.4:1 (v/v). In another embodiment, the ratio of EtOH:water may be 1.0:1.0. The mixture may be warmed to 35-40 °C and stirred for 30- 40 min, cooled to 13-17°C over a period of 60-120 min, and stirred at 13-17 °C for 60-90 min. If crystallization does not occur, the mixture may be seeded with tasimelteon (unmilled) crystals. Following addition of process water (e.g., 19.2 kg / kg of
Intermediate 5 (Stage 11) added over 2-2.5 hr at 10-15 °C followed by stirring at the same temperature for 60-90 min), the precipitate is collected by centrifugation and the cake is analyzed by HPLC to determine if the product meets pre-set specifications, e.g., tasimelteon NLT 99%, Impurities 5 and 6 NMT 0.15% a/a, and other individual impurities NMT 0.10% a/a, e.g., Impurities 1, 2, 3, 4, and 7. Material meeting said pre-set specifications is washed, e.g., with n-heptane, and then dried, e.g., until LOD is NMT 0.7%. The dried material is also analyzed for particle size. Material not meeting the preset specifications, e.g., for Impurities 5 and 6 is transferred back to the reaction vessel and recrystallized as described above, i.e., by re-dissolving in warm EtOH:water, filtering, allowing the mixture to cool and crystallize, further precipitating by slow addition of water and collecting by centrifugation. Such re-processed material that meets said impurity specifications is washed, dried and analyzed as described above, after which it is released for milling, discarded, or further re-processed.
The above-described end-step synthesis is illustrative only. For example, other organic solvents or mixtures thereof can be used in place of tert-butyl methyl ether (TBME).. Bases other than or in addition to NaOH can also be employed. The solvent for crystallization can be an aqueous solvent, such as an aqueous C1-C4 alcohol, e.g., methanol, ethanol, propanol, isopropanol, n-butanol, sec-butanol, isobutanol, or tert- butanol, or a mixture of organic solvents such as MTBE-EtOH-cyclohexane.
Tasimelteon drug substance is stored as the unmilled drug substance and milled on an as-needed basis, immediately prior to its use in capsule drug product manufacturing. It has been found that use of a jet mill and a dry nitrogen atmosphere is advantageous in achieving uniform particle size with good handling characteristics and minimal loss. Drug substance meeting particle size specifications (e.g., Do.i < 15 μιτι (i.e., 10% of the particles are 15 μιτι in diameter or less); Do.s < 30 μιη; Do.9 < 75 μιη for in process and (i) a D90 specification set at < 105 μηι; (ii) a D50 specification set at <45 μηι; and (iii) a D10 specification set at <15 μηι for release) is tightly sealed, e.g., in PE bags and/or aluminum bags, e.g., with a dessicant such as a silica dessicant.
When manufacturing pharmaceutical grade tasimelteon, i.e., tasimelteon that is intended for human use, good manufacturing practices (GMP) are employed such as may be required by regulatory bodies in relevant jurisdictions. Bulk pharmaceutical grade tasimelteon is then mixed with excipients to prepare bulk formulated tasimelteon and then formed into an appropriate pharmaceutical dosage form, such as capsules, each comprising 10 mg to 100 mg, e.g., 20 mg, of tasimelteon.
The description above refers to milling. However, the skilled person will recognize that other particle size reduction techniques, e.g., sieving, high shear fluid processing, etc., can also be employed. Similarly, milling techniques other than jet milling, e.g., grinding, cryogenic grinding, cutting or impacting, etc., can also be employed.
While the invention has been described in detail in connection with only a limited number of embodiments, it should be readily understood that the invention is not limited to such disclosed embodiments. Rather, the invention can be modified to incorporate any number of variations, alterations, substitutions or equivalent arrangements not heretofore described, but which are commensurate with the spirit and scope of the invention. Additionally, while various embodiments of the invention have been described, it is to be understood that aspects of the invention may include only some of the described embodiments. Accordingly, the invention is not to be seen as limited by the foregoing description, but is only limited by the scope of the appended claims.

Claims

CLAIMS What we claim is:
1. A process for synthesizing highly purified, pharmaceutical grade tasimelteon, the process comprising:
(a) propionylating ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) methanamine or a salt thereof to yield tasimelteon;
(b) crystallizing the tasimelteon produced in step (a);
(c) assaying the crystallized tasimelteon from step (b) for the presence of one or both of Impurity 5 (N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran- 4-yl) cyclopropyl) (propionamido)methyl) cyclopropyl) methyl) propionamide) and Impurity 6 (2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate) ; and
(d) (i) if the crystallized tasimelteon meets pre-set specifications for Impurity 5 or Impurity 6, or both, then collecting the highly purified, pharmaceutical grade tasimelteon or
(d) (ii) if the crystallized tasimelteon fails to meet pre-set specifications for Impurity 5 or Impurity 6, or both, then further purifying the tasimelteon and repeating steps (c) and (d), or discarding the batch.
2. The process of claim 1, wherein the propionylating step comprises contacting ((lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methanamine or a salt thereof with a propionyl halide, a propionyl anhydride, a propionyl ester, a propionyl amide, a propionyl imidazolide, or with propionic acid and a dehydrating agent or the product thereof.
3. The process of claim 2, wherein the propionylating step comprises contacting ((lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methanamine or a salt thereof with a propionyl halide, a propionyl anhydride, a propionyl ester, a propionyl amide, a propionyl imidazolide, or with propionic acid and a dehydrating agent or the product thereof in the presence of an organic solvent.
4. The process of claim 3, wherein the propionylating step comprises contacting
((lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methanamine or a salt thereof with propionyl chloride in the presence of an organic solvent and an aqueous base.
5. The process of claim 4, wherein the organic solvent comprises tert-butyl methyl ether (TBME) and the aqueous base comprises NaOH.
6. The process of claim 3, 4, or 5, wherein the ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl)methanamine or a salt thereof is Intermediate 5 (((lR,2R)-2-(2,3- dihydrobenzofuran-4-yl)cyclopropyl)methanaminium chloride) and wherein after the propionylation step and before the crystallizing step, the mixture of tasimelteon is assayed for the presence of Intermediate 5 and, if the mixture does not meet pre-set specifications for Intermediate 5, then repeating step (a) or discarding the mixture.
7. The process of claim 3, 4, 5, or 6, wherein after the propionylation step and before the crystallizing step, the mixture of tasimelteon is washed with aqueous base and the aqueous layer is discarded.
8. The process of claim 7, wherein the washed mixture is distilled and the distillate is discarded.
9. The process of claim 8, wherein the distilling step is carried out in ethanol at a pot temperature of up to about 58 °C and a pressure of less than about 100 mmHg.
10. The process of claim 1„ 2, 3, 4, 5, 6, 7, 8, or 9 wherein the crystallization step comprises dissolving the tasimelteon by stirring and warming a mixture of the tasimelteon and a C1-C4 alkanol.
11. The process of claim 10, wherein the mixture of C1-C4 alkanol and tasimelteon is warmed to about 35 to 40 °C while stirring and then cooled to about 13 to 17 °C while stirring.
12. The process of any of the preceding claims, wherein the crystallization step optionally comprises seeding.
13. The process of any of the preceding claims, wherein the assaying step is carried out by HPLC.
14. The process of any of the preceding claims, wherein the pre-set specifications for the one or both of Impurity 5 and Impurity 6 are each not more than 0.15% (Area/Area).
15. The process of any of the preceding claims, wherein the further purifying comprises recrystallizing the tasimelteon.
16. The process of claim 1, wherein the particle size of crystals collected in step (d) is reduced to meet particle size specifications for pharmaceutical grade tasimelteon.
17. The process of claim 16, wherein crystals that meet particle size specifications for pharmaceutical grade tasimelteon are admixed with one or more excipients to prepare a pharmaceutical composition comprising pharmaceutical grade tasimelteon.
18. A process for preparing a batch of highly purified, pharmaceutical grade
tasimelteon, the process comprising:
(a) analyzing a batch of tasimelteon synthesized under GMP conditions for the presence of one or more of:
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3- methylbutanamide (Impurity 1),
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide (Impurity 2),
• l,3-Bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea
(Impurity 3),
• N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4)
• N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl)cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5) , • 2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6),
• N-(((lR,2R)-2-(3-Oxo-2,3-dihydrobenzofuran-4- yl) cyclopropyl) methyl) propionamide (Impurity 7)
and
(b) if the batch meets pre-set specifications for the amount of the one or more of Impurity 1, Impurity 2, Impurity 3, Impurity 4, Impurity 5, Impurity 6, or Impurity 7, then continuing to process the tasimelteon to prepare bulk tasimelteon drug substance for formulation or
(c) if the tasimelteon does not meet said pre-set specifications, then further purifying (such as by recrystallization, trituration, extraction, or chromatography) the
tasimelteon and repeating steps (a) and (b) or discarding the batch.
19. The process of claim 18 wherein the pre-set specifications for each of the one or more impurities is NMT 0.15 wt%.
20. The process of claim 18 or 19 wherein the step (a) analysis is carried out by HPLC.
21. The process of claim 18 or 19 wherein step (a) comprises analyzing the batch for the presence of Impurity 3, Impurity 5, and Impurity 6 and wherein the step (a) analysis is carried out by HPLC.
22. The process of claim 21wherein step (a) comprises analyzing the batch for the presence of all of Impurity 1, Impurity 2, Impurity 3, Impurity 4, Impurity 5, Impurity 6, and Impurity 7 and wherein the step (a) analysis is carried out by HPLC.
23. The process of claim 18 or 19 wherein further pre-set specifications for continuing to process the tasimelteon comprise that the tasimelteon is NLT 95.0% pure by area.
24. The process of claim 23 wherein further pre-set specifications for continuing to process the tasimelteon include that the amount of any other single impurity is NMT 0.10 area%.
25. The process of claim 18, 19, 20, 21, or 22 wherein the step (b) processing of tasimelteon comprises reducing the tasimelteon particle size to meet particle size specifications.
26. The process of claim 25 wherein the particle size reduction is carried out using a jet mill under an inert gas (e.g., nitrogen, argon, or helium) and wherein the particle size specifications comprise one or more of (i) a D90 specification set at less than about 105 μπι,; (ii) a D50 specification set at less than about 45 μιη; and (iii) a D10 specification set at less than about 15 μιτι.
27. The process of claim 26 wherein the step (b) processing of tasimelteon further comprises admixing the milled tasimelteon with one or more pharmaceutically acceptable excipients to prepare tasimelteon bulk drug substance.
28. The process of claim 27, wherein the admixed tasimelteon is prepared for use in a pharmaceutical composition in pharmaceutical dosage units for human use.
29. The process of claim 18, 19, 20, 21, 22, 23, 24, or 25 wherein the batch of
tasimelteon that is analyzed in step (a) is synthesized by allowing ((lR,2R)-2-(2,3- dihydrobenzofuran-4-yl)cyclopropyl)methanaminium chloride (Intermediate 5) to come in contact and react with propionyl chloride in the presence of an organic solvent and a base.
30. The process of claim 29 wherein the tasimelteon synthesized by contacting and reacting ((1 R,2 R) -2 - (2, 3 -dihydrobenzofuran-4-yl) cyclopropyl) methanaminium chloride (Intermediate 5) with propionyl chloride in the presence of the base is then, prior to the step (a) analysis, prepared in crystalline form by filtering the reaction mixture to prepare a filtrate comprising the tasimelteon and then crystallizing the tasimelteon in a solvent.
31. The process of claim 30 wherein the solvent for the crystallization of tasimelteon is an aqueous alcohol, e.g., EtOH and water.
32. The process of claim 18, 19, 20, 21, 22, 23, 24, 25, 26, 27, 28, 29, or 30 wherein the solvent for the recrystallization of the tasimelteon is an aqueous alcohol, e.g., EtOH and water.
33. The process of claim 29, 30, 31, or 32 wherein the organic solvent is TBME and the base is NaOH.
34. The process of claim 30, 31, 32, or 33 wherein (i) the filtrate, prior to crystallizing, is concentrated by distillation,
(ii) an alcohol, e.g., EtOH, is added,
(iii) the residue/alcohol mixture is concentrated by distillation,
(iv) the residue is dissolved in an aqueous alcohol, e.g., EtOH and water,
(v) the tasimelteon is crystallized from the alcohol/water solution, and
(vi) the tasimelteon crystals are collected for the step (a) analysis.
35. The process of claim 34 wherein the step (c) recrystallization, if necessary, is carried out by subjecting the tasimelteon that failed to meet the pre-set specifications to steps (iv), (v), and (vi).
36. The process of claim 34 or 35 wherein the crystallization step (v) is facilitated by seeding.
37. A method of analyzing a batch of highly purified, pharmaceutical grade tasimelteon, the method comprising:
(a) providing a batch of tasimelteon synthesized under GMP conditions
(b) analyzing the batch of tasimelteon, using HPLC, for the presence of one or more of:
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3- methylbutanamide (Impurity 1),
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide (Impurity 2),
• l,3-Bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea
(Impurity 3), • N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4),
• N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5) ,
• 2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6),
• N-(((lR,2R)-2-(3-Oxo-2,3-dihydrobenzofuran-4- yl) cyclopropyl) methyl) propionamide (Impurity 7).
38. A process for preparing a batch of highly purified tasimelteon that comprises
(a) synthesizing a batch of tasimelteon in crystalline form; and
(b) analyzing the batch for the presence of one or more of
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3- methylbutanamide (Impurity 1),
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide (Impurity 2),
• l,3-Bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea
(Impurity 3),
• N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4)
• N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5) ,
• 2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6),
• N-(((lR,2R)-2-(3-Oxo-2,3-dihydrobenzofuran-4- yl) cyclopropyl) methyl) propionamide (Impurity 7).
and
(c) if the batch of tasimelteon comprises:
(i) NMT 0.15 wt% of the one or more of Impurities 1-7;
and
(ii) the batch comprises no more than 0.10 wt% of any single unidentified impurity; (d) milling the tasimelteon to meet particle size specifications or
(e) if the batch of tasimelteon does not meet the purity specifications recited in (c) (i) and (ii), then recrystallizing and reanalyzing the batch of tasimelteon.
39. A method for assessing the purity of a bulk tasimelteon composition, the method comprising:
(a) providing a standard batch of each of one or more of Impurities 1-7; and
(b) using the standard batches as a reference marker to determine the level of the one or more of Impurities 1-7 in the tasimelteon composition.
40. A batch of tasimelteon for use in preparing a pharmaceutical composition for human use, wherein the batch of tasimelteon comprises:
tasimelteon that is at least 98.0 area% pure and that has been analyzed and shown to comprise no more than 0.15 wt% of one or more of Impurities 1-7.
41. The method of claim 37, 38, or 39 wherein one or more of the following limitations apply:
the batch of tasimelteon is analyzed for compliance with pre-set specifications for each of the one or more impurities, said pre-set specifications being that none of the one or more impurities is present in an amount of more than 0.15 wt%;
the analysis is carried out by HPLC;
the analysis is carried out to detect the presence of all of Impurities 3, 5, and 6;
the analysis is carried out to detect the presence of all of Impurities 1, 2, 3, 4, 5, 6, and 7; the analysis comprises determining that the tasimelteon comprises at least 98.0 area% of the composition;
the analysis comprises determining that the amount of any other single impurity is NMT 0.10 area%.
42. Purified tasimelteon wherein the tasimelteon does not contain any of the following impurities at a concentration greater than about 0.15%:
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3- methylbutanamide (Impurity 1), • N-(((li?,2i?)-2-(2 -dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide (Impurity 2),
• l,3-Bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea
(Impurity 3),
• N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4)
• N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5) ,
• 2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6),
• N-(((lR,2R)-2-(3-Oxo-2,3-dihydrobenzofuran-4- yl) cyclopropyl) methyl) propionamide (Impurity 7).
43. The composition of claim 42, wherein the composition does not contain any other impurity at a concentration of greater than about 0.15%.
44. The tasimelteon of claim 42 wherein the tasimelteon does not contain any of the following impurities at a concentration greater than about 0.15% by weight:
• (+)-dehydroabietylamine or a salt thereof
• 2-(2,3-dihydrobenzofuran-4-yl)-cyclopropanecarboxylic acid or a salt thereof (Intermediate 3)
• (lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropane carboxamide
(Intermediate 4)
• ((li?,2i?)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) methanamine or a salt thereof (Intermediate 5)
• 4-vinyl-2,3-dihydrobenzofuran (VBF).
45. The tasimelteon of any of claims 42 through 44 that does not contain any related substance impurity at a concentration greater than about 0.1% by weight.
46. The tasimelteon of any of claims 42 through 45 does not contain ethyl diazoacetate at a concentration greater than about 10 ppm.
47. The tasimelteon of any of claims 42 through 46 that does not contain any of the following impurities at a concentration greater than about 20 ppm of propionyl chloride, propionyl anhydride, propionic acid, or ethyl propionate, individually or collectively.
48. The tasimelteon of any of claims 42 through 47 wherein the total amount of impurities is less than about 2.0%.
49. The tasimelteon of any of claims 42 through 48 that does not contain N-(((15,25)-2- (2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)propionamide at a concentration greater than about 0.4% relative to the total amount of both enantiomers of N-((2-(2,3- dihydrobenzofuran-4-yl)cyclopropyl)methyl)propionamide.
50. The tasimelteon of any of claims 42 through 49 prepared by the processes disclosed above.
51. A method of determining the purity of a batch of tasimelteon that comprises: a) obtaining a high performance liquid chromatogram or ultra-high performance liquid chromatogram of a sample of the batch;
b) identifying peaks in the chromatogram corresponding to impurities; and c) taking area measurements of the peaks to determine a relative concentration thereof,
said method also comprising:
(i) providing a standard batch of each of one or more of the following substances:
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-3- methylbutanamide (Impurity 1),
• N-(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)-pentanamide (Impurity 2),
• l,3-Bis(((li?,2i?)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methyl)urea
(Impurity 3),
• N-(((li?,2i?)-2-(benzofuran-4-yl)cyclopropyl)methyl)propionamide (Impurity 4) • N-((2-(2,3-dihydrobenzofuran-4-yl)-l-((2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) (propionamido) methyl) cyclopropyl) methyl) propionamide (Impurity 5) ,
• 2-hydroxy-6-(2-(propionamidomethyl)cyclopropyl)phenethyl 2-(2- hydroxy ethyl) -3 - (2- (propionamidomethyl) cyclopropyl) phenyl carbonate (Impurity 6),
• N-(((lR,2R)-2-(3-Oxo-2,3-dihydrobenzofuran-4- yl) cyclopropyl) methyl) propionamide (Impurity 7)
(ii) using the standard batches as reference markers to determine the elution characteristics of said substance under the chromatographic conditions used to analyze the tasimelteon composition.
52. A method of synthesizing tasimelteon, the method comprising:
contacting and reacting (lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropane carboxamide with a reducing agent and an acid in an organic solvent to prepare ((lR,2R)-2-(2,3-dihydrobenzofuran-4-yl)cyclopropyl)methanamine or a salt thereof; and
contacting and reacting the ((lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropyl) methanamine with a propionylating reagent to prepare tasimelteon.
53. The method of claim 52, wherein the reducing agent comprises LiAlH4.
54. The method of claim 52 or 53, wherein the acid comprises HC1
55. The method of claim 52, 53, or 54 wherein the organic solvent comprises TBME.
56. The method of claim 52, 53, 54, or 55 wherein the propionylating agent comprises propionyl chloride.
57. The method of claim 52, 53, 54, 55, or 56 wherein the propionylation step further includes an organic solvent and a base.
58. The method of claim 57, wherein the base comprises NaOH.
59. The method of claim 52, wherein the (lR,2R)-2-(2,3-dihydrobenzofuran-4- yl) cyclopropane carboxamide is reduced to prepare ((li?,2i?)-2-(2,3- dihydrobenzofuran-4-yl)cyclopropyl)methanamine or a salt thereof.
60. A composition comprising tasimelteon prepared by the process of any of claims 52- 58.
PCT/US2015/015564 2014-02-12 2015-02-12 Highly purified pharmaceutical grade tasimelteon WO2015123389A1 (en)

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EP18207420.3A EP3470405A1 (en) 2014-02-12 2015-02-12 Highly purified pharmaceutical grade tasimelteon
EP23167851.7A EP4223747A1 (en) 2014-02-12 2015-02-12 Highly purified pharmaceutical grade tasimelteon
EP15708063.1A EP3105212A1 (en) 2014-02-12 2015-02-12 Highly purified pharmaceutical grade tasimelteon
JP2016552281A JP6921534B2 (en) 2014-02-12 2015-02-12 High-purity pharmaceutical grade tasimelteon
US15/117,734 US10071977B2 (en) 2014-02-12 2015-02-12 Highly purifid pharmaceutical grade tasimelteon
US16/123,303 US10611744B2 (en) 2014-02-12 2018-09-06 Highly purified pharmaceutical grade tasimelteon
US16/800,721 US10829465B2 (en) 2014-02-12 2020-02-25 Highly purified pharmaceutical grade tasimelteon
US17/039,795 US11203581B2 (en) 2014-02-12 2020-09-30 Highly purified pharmaceutical grade tasimelteon
US17/455,308 US11566011B2 (en) 2014-02-12 2021-11-17 Highly purified pharmaceutical grade tasimelteon
US18/149,590 US11760740B2 (en) 2014-02-12 2023-01-03 Highly purified pharmaceutical grade tasimelteon
US18/362,073 US12049457B2 (en) 2014-02-12 2023-07-31 Highly purified pharmaceutical grade tasimelteon
US18/741,969 US20240336584A1 (en) 2014-12-04 2024-06-13 Highly purified pharmaceutical grade tasimelteon

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