Lucas Tobias, Dietz Jule-Philipp, Cardoso Flavio S P, Snead David R, Nelson Ryan C, Donsbach Kai O, Gupton B Frank, Opatz Till
Department of Chemistry, Johannes Gutenberg-University, Duesbergweg 10-14, 55128 Mainz, Germany.
Department of Chemical and Life Sciences Engineering, Virginia Commonwealth University, Richmond, Virginia 23284, United States.
Org Process Res Dev. 2023 Sep 5;27(9):1641-1651. doi: 10.1021/acs.oprd.3c00187. eCollection 2023 Sep 15.
An efficient gram-scale synthesis of the antituberculosis agent pretomanid using straightforward chemistry, mild reaction conditions, and readily available starting materials is reported. Four different protecting groups on the glycidol moiety were investigated for their technical feasibility and ability to suppress side reactions. Starting from readily available protected ()-glycidols and 2-bromo-4-nitro-1-imidazole, pretomanid could be prepared in a linear three-step synthesis in up to 40% isolated yield. In contrast to most syntheses reported so far, deprotection and cyclization were performed in a one-pot fashion without any hazardous steps or starting materials.
报道了一种使用直接的化学方法、温和的反应条件和容易获得的起始原料,高效克级合成抗结核药物pretomanid的方法。研究了缩水甘油部分的四种不同保护基团的技术可行性及其抑制副反应的能力。以容易获得的保护型()-缩水甘油和2-溴-4-硝基-1-咪唑为起始原料,pretomanid可通过线性三步合成法制备,分离产率高达40%。与迄今为止报道的大多数合成方法不同,脱保护和环化是在一锅法中进行的,没有任何危险步骤或起始原料。
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