Asano Keisuke, Matsubara Seijiro
Institute for Catalysis, Hokkaido University Sapporo, Hokkaido, 001-0021, Japan.
Department of Material Chemistry, Graduate School of Engineering, Kyoto University Kyotodaigaku-Katsura, Nishikyo, Kyoto, 615-8510, Japan.
Chem Rec. 2023 Jul;23(7):e202200200. doi: 10.1002/tcr.202200200. Epub 2022 Sep 26.
Three-dimensional organic structures containing sp carbons bearing four non-hydrogen substituents can provide drug-like molecules. Although such complex structures are challenging targets in synthetic organic chemistry, efficient synthetic approaches will open a new chemical space for pharmaceutical candidates. This review provides an account of our recent achievements in developing organocatalytic approaches to attractive molecular platforms based on optically active sp carbons integrating four different functional groups. These methodologies include asymmetric cycloetherification and cyanation of multifunctional ketones, both of which take advantage of the mild characteristics of organocatalytic activation. Enzyme-like but non-enzymatic organocatalytic systems can be used to precisely manufacture molecules containing complex chiral structures without substrate specificity problems. In addition, these catalytic systems control not only stereoselectivity but also site-selectivity and do not induce side reactions even from substrates with rich functionality.
含有带有四个非氢取代基的sp碳的三维有机结构可以提供类药物分子。尽管这类复杂结构在有机合成化学中是具有挑战性的目标,但高效的合成方法将为药物候选物开辟一个新的化学空间。本综述介绍了我们最近在开发基于整合四个不同官能团的光学活性sp碳的有吸引力的分子平台的有机催化方法方面所取得的成就。这些方法包括多功能酮的不对称环醚化和氰化反应,这两种反应都利用了有机催化活化的温和特性。类酶但非酶的有机催化体系可用于精确制造含有复杂手性结构的分子,而不存在底物特异性问题。此外,这些催化体系不仅控制立体选择性,还控制位点选择性,即使对于具有丰富官能团的底物也不会引发副反应。