Enantioselective Synthesis of Fluoxetine Hydrochloride

化学工业与工程

Chemcial Industry and Engineering

2008, Vol. 25

Issue (3) :251-258 DOI:

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Enantioselective Synthesis of Fluoxetine Hydrochloride

CAO He,LI Ai-jun,ZHOU Xue-qin,LIU Dong-zhi(School of Chemical Engineering and Technology,Tianjin University,Tianjin 300072,China)

(School of Chemical Engineering and Technology,Tianjin University,Tianjin 300072,China

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Abstract Fluoxetine hydrochloride is a potent and highly selective inhibitor of neutral serotonin-reuptake and is one of the most important drugs for the treatment of psychiatric disorders and metabolic problems.Due to its market value and the different pharmacological activities displayed by analogues of fluoxetine, several synthetic methods,including the enantioselective synthesis of both enantiomers,have been reported.Progress in enantioselective synthetic methods of fluoxetine hydrochloride were reviewed in this paper.

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Received 2008-05-15; published 2008-05-15

Cite this article:

CAO He,LI Ai-jun,ZHOU Xue-qin,LIU Dong-zhi.Enantioselective Synthesis of Fluoxetine Hydrochloride[J] Chemcial Industry and Engineering, 2008,V25(3): 251-258

[1]	��.5-��ɫ��Ƽ��͡[J].��ҽҩ:�ϳ�ҩ.��ҩ.�Ƽ��ֲ�,1996,17(1):32-34.
[2]	WONG D T,FULLE R W,ROBERTSON D W.Fluoxetineand its two enantiomers as selective serotonin-uptakeinhibitors[J].Acta Pharm Nord,1990,2(3):171-180.
[3]	ROBERTSON D W,KRUSHINSKI J H,FULLER R W,etal.Absolute configurations and pharmacological activities ofthe optical isomers of fluoxetine,a selective serotonin-uptake inhibitor[J].J Med Chem.1988,31(7):1-
[4]	ROBERTSON D W,JONES N D,SWARZENDRUBER JK,et al.Molecular-structure of fluoxetine hydrochloride,ahighly selective serotonin-uptake inhibitor[J].J MedChem,1988,31(1):185-189.
[5]	EFFLAND RICHARD C,KLEIN JOSEPH T.N-nitrosophenoxybenzenepropanamine and N-1-chloroethylcarbamate intermediates:US,5268468[P].1993-12-07.
[6]	CRNIC Z,KIRIN S I.N-substituted derivatives of N-methyl-3-(p-trifluoromethylphenoxy)-3-phenylpropylamineand the procedure for their preparation:US,5618968[P].1997-04-08.
[7]	REITER J,SIMIG G,MEZEI T,et al.Pharmaceuticalintermediate for the synthesis of fluoxetine and a process forthe preparation thereof:WO,0021917[P].2000-04-20.
[8]	WIRTH D D,MILLER M S,BOINI S K,et al.Identification and comparison of impurities in fluoxetinehydrochloride synthesized by seven different routes[J].OrgProcess Res Dev.2000,4(6):513-519
[9]	OHKUMA T,ISHII D,TAKENO H,et al.Asymmetrichydrogenation of amino ketones using chiral RuCl2(diphophine)(1,2-diamine)complexes[J].J Am ChemSoc,2000,122:6 510-6 511.
[10]	Sanyo Chemical Industries,Ltd.Preparation of betaaketoacid:JP,55151532[P].1980-11-26.
[11]	RIBEIRO J B,RAMOS M d C K V,de AQUINO NETO FR,et al.New microbiological catalytic accesses to(S)-fluoxetine[J].Catalysis Communications.2005,6(2):131-133
[12]	HUANG H L,LIU L T,CHEN S F,et al.The synthesis ofa chiral fluoxetine intermediate by catalytic enantioselectivehydrogenation of benzoylacetamide[J].TetrahedronAsymmetry,1998,9(10):1 637-1 640.
[13]	SORGER K,PETERSEN H,STOHRER J.Enantioselectivereformatsky process for preparing optically active alcohols,amines and derivatives thereof:US,6924386[P].2005-08-02.
[14]	FATIMA A,LAPIS A A M,PILLI R A.A concise totalsynthesis of(R)-fluoxetine,a potent and selective serotoninreuptake inhibitor[J].J Braz Chem Soc,2005,16(3A):495-499.
[15]	MILES W S,FIALCOWITZ E J,HALSTED E S.Enantiostereoselective synthesis of(S)-and(R)-fluoxetinehydrochloride[J].Tetrahedron,2001,57:9 925-9 929.
[16]	KUMER P,PANDEY R K.Process for the preparation ofenantiomericall pure 3-phenyl-3-hydroxypropylamine:US,6838581[P].2005-01-04.
[17]	PANDEY R K,FERNANDES R A,KUMA P.Anasymmetric dihydroxylation route to enantiomerically purenorfluoxetine and fluoxetine[J].Tetrahedron Letters,2002,43(25):4 425-4 426.
[18]	GAO Y,KLUNDER J M,HANSON R M,et al.Catalyticasymmetric epoxidation and kinetic resolution:Modifiedprocedures including in situ derivatization[J].J Am ChemSoc,1987,109(19):5 765-5 780.
[19]	GAO Y,SHARPLESS K B.Asymmetric synthesis of bothenantiomers of tomoxetine and fluoxetine.Selectivereduction of 2,3-epoxycinnamyl alcohol with Red-Al[J].JOrg Chem,1988,53(17):4 081-4 088.
[20]	HILBORN J W,LU Z H,JURGENS A R,et al.Apractical asymmetric synthesis of(R)-fluoxetine and itsmajor metabolite(R)-norfluoxetine[J].TetrahedronLetters,2001,42(51):8 919-8 921.
[21]	KAKEI H,NEMOTO T,OHSHIMA T,et al.Efficientsthesis of ciral-��and-��hydroxy amides:Application to thesnthesis of R)-fluoxetine[J].Angew Chem Int Ed.2004,43(3):317-320
[22]	WANG G,LIU X,ZHAO G.Polymer-supported chiralsulfonamide catalyzed one-pot reduction of-��keto nitriles:A practical synthesis of(R)-fluoxetine and(R)-duloxetine[J].Tetrahedron Asymmetry.2005,16(10):1-
[23]	PANUNZIO M,ROSSI K,TAMANINI E,et al.Synthesisof enantiomerically pure(S)-and(R)-fluoxetine(Prozac)via a hetero Diels-Alder strategy[J].TetrahedronAsymmetry,2004,15(22):3 489-3 493.
[24]	HIBORN J W,JURGENS A R.Fluoxetine process frombenzoylacetonitrile:US,6025517[P].2000-02-15.
[25]	BROWN H C.Process for producing optically pure 2-phenoxyphenylalkylamines:US,5068432[P].1991-11-26.
[26]	SREBNIK M,RAMACHANDRAN P V,BROWN H C.Chiral synthesis via organoboranes.18.Selective reductions.43.Diisopinocampheylchloroborane as an excellent chiralreducing reagent for the synthesis of halo alcohols of highenantiomeric purity.A highly enantioselective synthesis ofboth optical isomers of tomoxetine,fluoxetine,andnisoxetine[J].J Org Chem,1988,53(13):2 916-2 920.