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      A Novel Convergent Synthesis of the Potent Antiglaucoma Agent Tafluprost

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          Abstract

          Tafluprost (AFP-168, 5) is a unique 15-deoxy-15,15-difluoro-16-phenoxy prostaglandin F 2α (PGF ) analog used as an efficacious ocular hypotensive agent in the treatment of glaucoma and ocular hypertension, as monotherapy, or as adjunctive therapy to β-blockers. A novel convergent synthesis of 5 was developed employing Julia–Lythgoe olefination of the structurally advanced prostaglandin phenylsulfone 16, also successfully applied for manufacturing of pharmaceutical grade latanoprost ( 2), travoprost ( 3) and bimatoprost ( 4), with an aldehyde ω-chain synthon 17. The use of the same prostaglandin phenylsulfone 16, as a starting material in parallel syntheses of all commercially available antiglaucoma PGF analogs 25, significantly reduces manufacturing costs resulting from its synthesis on an industrial scale and development of technological documentation. Another key aspect of the route developed is deoxydifluorination of a trans-13,14-en-15-one 30 with Deoxo-Fluor. Subsequent hydrolysis of protecting groups and final esterification of acid 6 yielded tafluprost ( 5). The main advantages are the preparation of high purity tafluprost ( 5) and the application of comparatively cheap reagents. The preparation and identification of two other tafluprost acid derivatives, tafluprost methyl ester ( 32) and tafluprost ethyl amide ( 33), are also described.

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          Readily accessible 12-I-5 oxidant for the conversion of primary and secondary alcohols to aldehydes and ketones

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            Syntheses a l'aide de sulfones v(+)- methode de synthese generale de doubles liaisons.

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              Stereo-controlled synthesis of dl-prostaglandins F2.alpha. and E2

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                Author and article information

                Contributors
                Role: Academic Editor
                Journal
                Molecules
                Molecules
                molecules
                Molecules : A Journal of Synthetic Chemistry and Natural Product Chemistry
                MDPI
                1420-3049
                31 January 2017
                February 2017
                : 22
                : 2
                : 217
                Affiliations
                [1 ]R & D Chemistry Department, Pharmaceutical Research Institute, Rydygiera 8, 01-793 Warsaw, Poland; m.krupa@ 123456ifarm.eu (M.K.); m.chodynski@ 123456ifarm.eu (M.C.); a.ostaszewska@ 123456ifarm.eu (A.O.); piotr.cmoch@ 123456icho.edu.pl (P.C.)
                [2 ]Institute of Organic Chemistry, Polish Academy of Sciences, Kasprzaka 42/52, 01-224 Warsaw, Poland
                Author notes
                [* ]Correspondence: dams@ 123456ifarm.eu ; Tel.: +48-22-456-3929; Fax: +48-22-456-3838
                Article
                molecules-22-00217
                10.3390/molecules22020217
                6155834
                28146132
                7539dc04-d116-43cb-83ef-3629dc3a20fb
                © 2017 by the authors.

                Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license ( http://creativecommons.org/licenses/by/4.0/).

                History
                : 05 December 2016
                : 25 January 2017
                Categories
                Article

                tafluprost,prostaglandins,corey lactone,julia–lythgoe olefination,fluorination

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