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利用定制亲核探针实现蛋白质反应性天然产物的亚类特异性标记。

Subclass-specific labeling of protein-reactive natural products with customized nucleophilic probes.

作者信息

Rudolf Georg C, Koch Maximilian F, Mandl Franziska A M, Sieber Stephan A

机构信息

Center for Integrated Protein Science CIPSM, Institute of Advanced Studies IAS, Department Chemie, Lehrstuhl für Organische Chemie II, Technische Universität München, Lichtenbergstrasse 4, 85747 Garching (Germany).

出版信息

Chemistry. 2015 Feb 23;21(9):3701-7. doi: 10.1002/chem.201405009. Epub 2015 Jan 21.

Abstract

Natural products represent a rich source of bioactive compounds that constitute a large fraction of approved drugs. Among those are molecules with electrophilic scaffolds, such as Michael acceptors, β-lactams, and epoxides that irreversibly inhibit essential enzymes based on their catalytic mechanism. In the search for novel bioactive molecules, current methods are challenged by the frequent rediscovery of known chemical entities. Herein small nucleophilic probes that attack electrophilic natural products and enhance their detection by HPLC-UV and HPLC-MS are introduced. A screen of diverse probe designs revealed one compound with a desired selectivity for epoxide- and maleimide-based antibiotics. Correspondingly, the natural products showdomycin and phosphomycin could be selectively targeted in extracts of their natural producing organism, in which the probe-modified molecules exhibited superior retention and MS detection relative to their unmodified counterparts. This method may thus help to discover small, electrophilic molecules that might otherwise easily elude detection in complex samples.

摘要

天然产物是生物活性化合物的丰富来源,这些化合物构成了大量已批准药物的一部分。其中包括具有亲电支架的分子,如迈克尔受体、β-内酰胺和环氧化物,它们基于催化机制不可逆地抑制必需酶。在寻找新型生物活性分子的过程中,目前的方法面临着频繁重新发现已知化学实体的挑战。在此介绍了攻击亲电天然产物并通过HPLC-UV和HPLC-MS增强其检测的小亲核探针。对多种探针设计的筛选揭示了一种对基于环氧化物和马来酰亚胺的抗生素具有所需选择性的化合物。相应地,天然产物showdomycin和磷霉素可以在其天然产生生物体的提取物中被选择性靶向,其中探针修饰的分子相对于未修饰的对应物表现出更好的保留和质谱检测。因此,这种方法可能有助于发现小的亲电分子,否则这些分子在复杂样品中可能很容易逃脱检测。

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