Inhibition of chaperone-dependent bacterial ribosome biogenesis.

Abdalla Al Refaii, Jean-Hervé Alix
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引用次数: 3

Abstract

In Escherichia coli, the molecular chaperone HSP70 (DnaK) is necessary for 30S and 50S ribosomal subunit assembly at temperatures above 37 degrees C. Inhibitors of DnaK should therefore hinder ribosome biogenesis, in addition to all of the other DnaK-dependent cellular functions. An easily testable phenotype of DnaK is described here based on alpha-complementation of beta-galactosidase. This protein fragment complementation requires a functional DnaK in vivo, offering a suitable method for screening for DnaK inhibitors. Subsequently, it will be of great importance to check whether inhibitors of bacterial DnaK selected in this way have an effect (inhibitory or stimulatory) on the activities of eukaryotic HSP70 and HSC70 chaperones, because of the universal conservation in all biota of these chaperones in both their structural and functional properties. This question is important due to their implication in many pathways in immunology, cancer biology, and neurodegenerative disorders.

伴侣依赖细菌核糖体生物发生的抑制作用。
在大肠杆菌中,分子伴侣HSP70 (DnaK)是在37℃以上温度下30S和50S核糖体亚基组装所必需的。因此,除了所有其他依赖dna的细胞功能外,DnaK的抑制剂还会阻碍核糖体的生物发生。这里描述了一种易于测试的DnaK表型,该表型基于β -半乳糖苷酶的α -互补。这种蛋白质片段互补需要在体内具有功能的DnaK,为筛选DnaK抑制剂提供了合适的方法。因此,检查以这种方式选择的细菌DnaK抑制剂是否对真核HSP70和HSC70伴侣蛋白的活性有影响(抑制或刺激)将是非常重要的,因为这些伴侣蛋白的结构和功能特性在所有生物群中都是普遍保守的。这个问题很重要,因为它们在免疫学、癌症生物学和神经退行性疾病的许多途径中都有意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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