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基于作用机制检测亲电天然产物的硫醇探针

Thiol Probes To Detect Electrophilic Natural Products Based on Their Mechanism of Action.

作者信息

Castro-Falcón Gabriel, Hahn Dongyup, Reimer Daniela, Hughes Chambers C

机构信息

Center for Marine Biotechnology and Biomedicine, Scripps Institution of Oceanography, University of California, San Diego , La Jolla, California 92093, United States.

出版信息

ACS Chem Biol. 2016 Aug 19;11(8):2328-36. doi: 10.1021/acschembio.5b00924. Epub 2016 Jun 28.

Abstract

New methods are urgently needed to find novel natural products as structural leads for the development of new drugs against emerging diseases such as cancer and multiresistant bacterial infections. Here we introduce a reactivity-guided drug discovery approach for electrophilic natural products, a therapeutically relevant class of natural products that covalently modify their cellular targets, in crude extracts. Using carefully designed halogenated aromatic reagents, the process furnishes derivatives that are UV-active and highly conspicuous via mass spectrometry by virtue of an isotopically unique bromine or chlorine tag. In addition to the identification of high-value metabolites, the process facilitates the difficult task of structure elucidation by providing derivatives that are primed for X-ray crystallographic analysis. We show that a cysteine probe efficiently and chemoselectively labels enone-, β-lactam-, and β-lactone-based electrophilic natural products (parthenolide, andrographolide, wortmannin, penicillin G, salinosporamide), while a thiophenol probe preferentially labels epoxide-based electrophilic natural products (triptolide, epoxomicin, eponemycin, cyclomarin, salinamide). Using the optimized method, we were able to detect and isolate the epoxide-bearing natural product tirandalydigin from Salinispora and thereby link an orphan gene cluster to its gene product.

摘要

迫切需要新方法来寻找新型天然产物,作为开发针对癌症和多重耐药细菌感染等新兴疾病的新药的结构先导物。在此,我们介绍一种针对亲电天然产物的反应性导向药物发现方法,亲电天然产物是一类具有治疗相关性的天然产物,可在粗提物中与细胞靶点发生共价修饰。使用精心设计的卤代芳香试剂,该过程可提供通过质谱具有紫外线活性且因同位素独特的溴或氯标签而高度显著的衍生物。除了鉴定高价值代谢物外,该过程还通过提供适合X射线晶体学分析的衍生物,促进了结构解析这一艰巨任务。我们表明,半胱氨酸探针能有效且化学选择性地标记基于烯酮、β-内酰胺和β-内酯的亲电天然产物(小白菊内酯、穿心莲内酯、渥曼青霉素、青霉素G、盐孢菌素),而苯硫酚探针则优先标记基于环氧化物的亲电天然产物(雷公藤内酯醇、环氧霉素、埃博霉素、环马林、盐霉素)。使用优化后的方法,我们能够从盐孢菌中检测并分离出含环氧化物的天然产物替兰地吉菌素,从而将一个孤儿基因簇与其基因产物联系起来。

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