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仿生方法从生物合成支架中获得多样的珊瑚二萜。

Biomimetic Approach to Diverse Coral Diterpenes from a Biosynthetic Scaffold.

机构信息

Department of Medicinal Chemistry, University of Utah, 30 South 2000 East, Salt Lake City, UT 84112, USA.

出版信息

Angew Chem Int Ed Engl. 2023 Sep 25;62(39):e202311406. doi: 10.1002/anie.202311406. Epub 2023 Aug 24.

Abstract

Thousands of coral terpenes originate from simple scaffolds that undergo oxidative tailoring. While corals are excellent sources of drug leads, the challenge of supplying structurally complex drug leads from marine organisms has sometimes slowed their development. Making this even more challenging, in comparison to other organisms, such as plants and microbes, for which the terpene literature is substantial, very little is known about how the unique coral terpenes are biosynthesized and elaborated in nature. In this study, we used a semisynthetic strategy to produce at gram scale in yeast the eunicellane scaffold that underlies >200 coral compounds. Synthetic oxidation reactions were explored, generating key scaffolds that reflect three of the four structural classes derived from eunicellane and enabling the first asymmetric syntheses of the natural products solenopodin C and klysimplexin Q. Biomimetic methods and detailed mechanistic studies of synthetic reactions shed light on potential enzymological reactivity, including the role of epoxide rearrangement in eunicellane biosynthesis.

摘要

数千种珊瑚萜类化合物起源于简单的支架,这些支架经历了氧化修饰。虽然珊瑚是药物先导的极好来源,但从海洋生物中供应结构复杂的药物先导的挑战有时会减缓它们的发展。与其他生物体相比,这更具挑战性,因为与植物和微生物等生物体相比,萜类文献非常丰富,而对于珊瑚萜类化合物在自然界中是如何生物合成和修饰的,人们知之甚少。在这项研究中,我们使用半合成策略在酵母中以克为单位生产了基础超过 200 种珊瑚化合物的 eunicellane 支架。我们探索了合成氧化反应,生成了反映源自 eunicellane 的四个结构类别中的三个的关键支架,并首次实现了天然产物 solenopodin C 和 klysimplexin Q 的不对称合成。仿生方法和对合成反应的详细机制研究揭示了潜在的酶反应性,包括环氧重排在 eunicellane 生物合成中的作用。

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