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通过多种磺酰氟的统一合成实现布氏锥虫抑制剂的发现。

Discovery of Trypanosoma brucei inhibitors enabled by a unified synthesis of diverse sulfonyl fluorides.

作者信息

Mantilla Brian S, White Jack S, Mosedale William R T, Gomm Andrew, Nelson Adam, Smith Terry K, Wright Megan H

机构信息

School of Chemistry and Astbury Centre for Structural Molecular Biology, University of Leeds, Leeds, LS2 9JT, UK.

Schools of Biology and Chemistry, Biomedical Sciences Research Complex, University of St Andrews, St Andrews, KY16 9ST, UK.

出版信息

Commun Chem. 2024 Oct 19;7(1):237. doi: 10.1038/s42004-024-01327-8.

Abstract

Sets of electrophilic probes are generally prepared using a narrow toolkit of robust reactions, which tends to limit both their structural and functional diversity. A unified synthesis of skeletally-diverse sulfonyl fluorides was developed that relied upon photoredox-catalysed dehydrogenative couplings between hetaryl sulfonyl fluorides and hydrogen donor building blocks. A set of 32 diverse probes was prepared, and then screened against Trypanosoma brucei. Four of the probes were found to have sub-micromolar anti-trypanosomal activity. A chemical proteomic approach, harnessing an alkynylated analogue and broad-spectrum fluorophosphonate tools, provided insights into the observed anti-trypanosomal activity, which likely stems from covalent modification of multiple protein targets. It is envisaged that the unified diversity-oriented approach may enable the discovery of electrophilic probes that have value in the elucidation of biological and biomedical mechanisms.

摘要

亲电探针集通常使用一套有限的稳健反应来制备,这往往会限制它们的结构和功能多样性。开发了一种统一的合成方法,用于合成骨架多样的磺酰氟,该方法依赖于杂芳基磺酰氟与氢供体结构单元之间的光氧化还原催化脱氢偶联反应。制备了一组32种不同的探针,然后针对布氏锥虫进行筛选。发现其中四种探针具有亚微摩尔级的抗锥虫活性。一种化学蛋白质组学方法,利用炔基化类似物和广谱氟膦酸盐工具,为观察到的抗锥虫活性提供了深入见解,这种活性可能源于对多个蛋白质靶点的共价修饰。可以设想,这种统一的多样性导向方法可能有助于发现对阐明生物学和生物医学机制有价值的亲电探针。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3fac/11490619/ed07bc048210/42004_2024_1327_Fig1_HTML.jpg

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