Adachi Shinya, Cognetta Armand B, Niphakis Micah J, He Zhi, Zajdlik Adam, St Denis Jeffrey D, Scully Conor C G, Cravatt Benjamin F, Yudin Andrei K
Davenport Research Laboratories, Department of Chemistry, University of Toronto, 80 St. George St., Toronto, ON M5S3H6, Canada.
Chem Commun (Camb). 2015 Feb 28;51(17):3608-11. doi: 10.1039/c4cc09107h.
The discovery of enzyme inhibitors relies on synthetic methods that enable rapid and modular construction of small molecules. Heterocyclic fragments designed to maximize enthalpic interactions with their protein targets represent a particularly desirable class of molecules. Here we describe a reagent that enables straightforward construction of "borofragments", in which a heterocycle is separated from the boron center by two or three rotatable bonds. The stability of these molecules depends on the MIDA group which likely acts as a slow-release element under biological conditions. Borofragments can be used to discover inhibitors of enzymes that use catalytic oxygen nucleophiles. We have employed this method to identify inhibitors of ABHD10 and the predicted carboxypeptidase CPVL. This technique should be applicable to other classes of targets.
酶抑制剂的发现依赖于能够快速且模块化构建小分子的合成方法。设计用于最大化与蛋白质靶点焓相互作用的杂环片段代表了一类特别理想的分子。在此,我们描述了一种试剂,它能够直接构建“硼片段”,其中杂环通过两个或三个可旋转键与硼中心分离。这些分子的稳定性取决于MIDA基团,该基团在生物条件下可能充当缓释元素。硼片段可用于发现使用催化氧亲核试剂的酶的抑制剂。我们已采用此方法鉴定ABHD10和预测的羧肽酶CPVL的抑制剂。该技术应适用于其他类别的靶点。
