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用于鉴定靶向特定翻译步骤的抑制剂的检测方法。

Assays for the identification of inhibitors targeting specific translational steps.

作者信息

Brandi Letizia, Dresios John, Gualerzi Claudio O

机构信息

Department of Biology MCA, University of Camerino, Camerino, MC, Italy.

出版信息

Methods Mol Med. 2008;142:87-105. doi: 10.1007/978-1-59745-246-5_8.

Abstract

While bacterial protein synthesis is the target of about half of the known antibiotics, the great structural-functional complexity of the translational machinery still offers remarkable opportunities for identifying novel and specific inhibitors of unexploited targets. We designed a knowledge-based in vitro translation assay to identify inhibitors selectively targeting the bacterial or the yeast translational apparatus, preferentially blocking the early steps of protein synthesis. Using a natural-like, "universal" model mRNA and cell-free extracts prepared from Eschericha coli, Saccharomyces cerevisiae, and HeLa cells, we were able to translate, with comparable yields in the three systems, the immunogenic peptide encoded by this "universal" mRNA. The immuno-enzymatic quantification of the translated peptide in the presence of a potential inhibitor can identify a selective bacterial or fungal inhibitor inactive in the human system. When applied to the high-throughput screening (HTS) of a library of approximately 25,000 natural products, this assay led to the identification of two novel and specific inhibitors of bacterial translation.

摘要

虽然细菌蛋白质合成是约一半已知抗生素的作用靶点,但翻译机制巨大的结构-功能复杂性仍为鉴定未开发靶点的新型特异性抑制剂提供了显著机会。我们设计了一种基于知识的体外翻译试验,以鉴定选择性靶向细菌或酵母翻译装置的抑制剂,优先阻断蛋白质合成的早期步骤。使用一种类似天然的“通用”模型mRNA以及从大肠杆菌、酿酒酵母和人宫颈癌细胞系(HeLa细胞)制备的无细胞提取物,我们能够在这三种系统中以相当的产量翻译由这种“通用”mRNA编码的免疫原性肽。在存在潜在抑制剂的情况下对翻译肽进行免疫酶定量,可以鉴定出在人体系统中无活性的选择性细菌或真菌抑制剂。当将该试验应用于对约25000种天然产物文库的高通量筛选(HTS)时,鉴定出了两种新型的细菌翻译特异性抑制剂。

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