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Multilevel structure–activity profiling reveals multiple green tea compound families that each modulate ubiquitin-activating enzyme and ubiquitination by a distinct mechanism

机译:多级结构-活性分析揭示了多个绿茶化合物家族每个家族均通过独特的机制调节泛素激活酶和泛素化

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摘要

We developed and implemented a reconstituted system to screen for modulators of the ubiquitination of proliferating cell nuclear antigen, a process that activates pathways of DNA damage tolerance and drug resistance. We identified the primary putatively health-beneficial green tea polyphenol epigallocatechin gallate (EGCG) and certain related small molecules as potent inhibitors of ubiquitination. EGCG directly and reversibly targets the ubiquitin-activating enzyme Uba1, blocking formation of the Uba1~ubiquitin thioester conjugate and thus ubiquitination and in the cell. Structure–activity relationship profiles across multiple biochemical and cellular assays for a battery of EGCG analogues revealed distinct chemical and mechanism-of-action clusters of molecules, with catechin gallates, alkyl gallates, and myricetin potently inhibiting ubiquitination. This study defines a number of related though distinct first-in-class inhibitors of ubiquitination, each series with its own unique activity pattern and mechanistic signature.
机译:我们开发并实施了重组系统,以筛选增殖细胞核抗原泛素化的调节剂,该过程可激活DNA损伤耐受性和耐药性途径。我们确定了主要的有益健康的绿茶多酚表没食子儿茶素没食子酸酯(EGCG)和某些相关的小分子作为泛素化的有效抑制剂。 EGCG直接和可逆地靶向泛素激活酶Uba1,阻止Uba1-泛素硫酯缀合物的形成,从而阻止泛素化并在细胞内形成。一系列EGCG类似物在多种生化和细胞测定中的结构-活性关系概况揭示了分子的独特化学和作用机理簇,儿茶素没食子酸酯,烷基没食子酸酯和杨梅素有效抑制泛素化。这项研究定义了许多相关的,尽管不同的一流的泛素化抑制剂,每个系列都有其自己独特的活性模式和机制特征。

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