Process development and scale-up of the PPAR agonist NNC 61-4655

…, B Weber, V Weil, SJ Mozer, P Sauerberg

文献索引：Deussen, Heinz-Josef; Jeppesen, Lone; Schaerer, Norbert; Junager, Finn; Bentzen, Bjorn; Weber, Beat; Weil, Volker; Mozer, Sandor Josef; Sauerberg, Per Organic Process Research and Development, 2004 , vol. 8, # 3 p. 363 - 371

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被引用次数: 24

摘要

A scalable synthetic route of the nonselective but PPARα-preferring potent PPAR agonist NNC 61-4655 aimed for treatment of type 2 diabetes was developed. The synthetic pathway comprises the convergent synthesis and coupling of the two key intermediates E-5- (chloropent-3-en-1-ynyl) benzene 8 (prepared in a five-step synthesis in 18% overall yield) and (S)-2-ethoxy-3-(4-hydroxyphenyl) propanoic acid isopropyl ester 9. The 2- ...

197299-16-4

2-乙氧基-3-对羟基苯基丙酸乙酯

~47%

325793-65-5

(S)-2-乙氧基-3-(4-...

~38%

Synthesis and biological and structural characterization of ...

[Journal of Medicinal Chemistry, , vol. 46, # 8 p. 1306 - 1317]

Claisen Condensation as a Facile Route to an α-Alkoxy-cinnam...

[Organic Process Research and Development, , vol. 8, # 6 p. 838 - 845]

Claisen Condensation as a Facile Route to an α-Alkoxy-cinnam...

[Linderberg, Mats T.; Moge, Mikael; Sivadasan, Sivaprasad Organic Process Research and Development, 2004 , vol. 8, # 6 p. 838 - 845]

Claisen Condensation as a Facile Route to an α-Alkoxy-cinnam...

[Organic Process Research and Development, , vol. 8, # 6 p. 838 - 845]