探索用于合成异卡前列素和15R-16-(间甲苯基)-17,18,19,20-四去甲异卡前列素的ω-侧链添加策略。
Exploration of omega-side chain addition strategies for the syntheses of isocarbacyclin and 15R-16-(m-tolyl)-17,18,19,20-tetranorisocarbacyclin.
作者信息
Sheddan Neil A, Mulzer Johann
机构信息
Institut für Organische Chemie der Universität Wien, Wien, Austria.
出版信息
Org Biomol Chem. 2006 Nov 21;4(22):4127-30. doi: 10.1039/b611339g.
We describe alternative access to prostacyclin analogues by means of two omega-side chain addition strategies: Grignard reagent addition to an alpha,beta-unsaturated Weinreb amide, followed by diastereoselective reduction of the corresponding enone system, and implementation of Seebach's alkylation chemistry. These strategies have led to the syntheses of biologically active prostacyclin analogues isocarbacyclin and 15R- 16-(m-tolyl)- 17,18,19,20-tetranorisocarbacyclin (15R-TIC), with modest to excellent diastereoselectivity.
我们描述了通过两种ω-侧链添加策略来获得前列环素类似物的替代方法:格氏试剂加成到α,β-不饱和Weinreb酰胺上,随后对相应的烯酮体系进行非对映选择性还原,以及实施Seebach的烷基化化学方法。这些策略已导致合成具有适度至优异非对映选择性的生物活性前列环素类似物异环前列素和15R-16-(间甲苯基)-17,18,19,20-四去甲异环前列素(15R-TIC)。
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