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用于生成人类羧酸酯酶抑制剂的含1,2 - 二酮的枞酸型类似物的简便合成方法。

Facile synthesis of 1,2-dione-containing abietane analogues for the generation of human carboxylesterase inhibitors.

作者信息

Binder Randall J, Hatfield M Jason, Chi Liying, Potter Philip M

机构信息

Department of Chemical Biology and Therapeutics, 262 Danny Thomas Place, St. Jude Children's Research Hospital, Memphis, TN 38105, United States.

出版信息

Eur J Med Chem. 2018 Apr 10;149:79-89. doi: 10.1016/j.ejmech.2018.02.052. Epub 2018 Feb 19.

Abstract

Recently, a series of selective human carboxylesterase inhibitors have been identified based upon the tanshinones, with biologically active molecules containing a 1,2-dione group as part of a naphthoquinone core. Unfortunately, the synthesis of such compounds is complex. Here we describe a novel method for the generation of 1,2-dione containing diterpenoids using a unified approach, by which boronic acids are joined to vinyl bromo-cyclohexene derivatives via Suzuki coupling, followed by electrocyclization and oxidation to the o-phenanthroquinones. This has allowed the construction of a panel of miltirone analogues containing an array of substituents (methyl, isopropyl, fluorine, methoxy) which have been used to develop preliminary SAR with the two human carboxylesterase isoforms. As a consequence, we have synthesized highly potent inhibitors of these enzymes (K < 15 nM), that maintain the core tanshinone scaffold. Hence, we have developed a facile and reproducible method for the synthesis of abietane analogues that have resulted in a panel of miltirone derivatives that will be useful tool compounds to assess carboxylesterase biology.

摘要

最近,基于丹参酮已鉴定出一系列选择性人羧酸酯酶抑制剂,其生物活性分子含有作为萘醌核心一部分的1,2 - 二酮基团。不幸的是,此类化合物的合成很复杂。在此,我们描述了一种使用统一方法生成含1,2 - 二酮二萜类化合物的新方法,通过该方法硼酸经铃木偶联与乙烯基溴代环己烯衍生物连接,随后进行电环化并氧化为邻菲醌。这使得能够构建一组含有一系列取代基(甲基、异丙基、氟、甲氧基)的丹参酮类似物,这些类似物已用于与两种人羧酸酯酶同工型开展初步的构效关系研究。因此,我们合成了这些酶的高效抑制剂(K<15 nM),其保留了核心丹参酮骨架。所以,我们开发了一种简便且可重复的方法来合成松香烷类似物,该方法已得到一组丹参酮衍生物,这些衍生物将成为评估羧酸酯酶生物学的有用工具化合物。

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