Practical Manufacturing Process for Baloxavir Marboxil: Effective Selection and Replacement of Protective Group toward Enhancement of Crystallization-Induced Diastereomer Transformation

Nobuaki Fukui, Setsuya Shibahara, Toshikatsu Maki, Tatsuhiko Ueno, Shuichi Yanagisawa,Kazuya Okamoto, Emi Tanimoto,Takafumi Ohara,Tatsuro Yasukata,Takayuki Tsuritani

ORGANIC PROCESS RESEARCH & DEVELOPMENT(2024)

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摘要
Baloxavir marboxil (BXM) is an influenza antiviral drug that exploits a cap-dependent endonuclease (CEN) inhibitor. The synthesis route used in the initial CMC development study had several problems hampering scale-up, such as poor stereochemical outcome which decreased the yield, usage of a corrosive reagent, and a cumbersome protocol for the key step. We addressed these problems to enable practical and operation-friendly manufacture of BXM at a larger production scale for early and successive CMC development. The new route includes the following steps: (1) a magnesium-mediated alkoxy displacement reaction to prepare an intermediate without loss of optical purity and (2) diastereoselective preparation of an intermediate via a dehydration condensation reaction with a crystallization-induced diastereomer transformation (CIDT) process. This facile route enabled scalable manufacturing to supply BXM.
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关键词
baloxavir marboxil,S-033188,influenza antiviral,scalable process,crystallization-induced diastereomertransformation (CIDT),magnesium alkoxide,transesterification,condensation reaction
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