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线粒体前导序列中Tom20结合片段的核磁共振鉴定

NMR identification of the Tom20 binding segment in mitochondrial presequences.

作者信息

Muto T, Obita T, Abe Y, Shodai T, Endo T, Kohda D

机构信息

Department of Structural Biology, Biomolecular Engineering Research Institute, Suita, 565-0874, Japan.

出版信息

J Mol Biol. 2001 Feb 16;306(2):137-43. doi: 10.1006/jmbi.2000.4397.

Abstract

Many mitochondrial proteins are synthesized in the cytosol as precursors with N-terminal presequences, and are imported into mitochondria with the aid of translocator protein complexes containing presequence-binding proteins. Tom20, a receptor protein which functions in an early step of the mitochondrial protein import, recognizes presequences with divergent amino acid sequences. Here, we report the identification of the segments involved in binding to Tom20 in mitochondrial presequences. We monitored the chemical shift perturbation of the NMR signals of five different 15N-labeled presequence peptides by the addition of the cytosolic receptor domain of rat or yeast Tom20. The perturbed segments occupy different positions, either near the N terminus or at the C terminus, in the presequences. Spin label experiments revealed that this is not due to different orientations of the presequence peptides bound to Tom20. The results presented here will offer a starting point to perform detailed analyses of Tom20-binding elements by systematic amino acid replacements.

摘要

许多线粒体蛋白在胞质溶胶中以前体形式合成,带有N端前导序列,并在含有前导序列结合蛋白的转运蛋白复合物的帮助下导入线粒体。Tom20是一种在线粒体蛋白导入早期步骤中起作用的受体蛋白,它能识别具有不同氨基酸序列的前导序列。在此,我们报告了线粒体前导序列中与Tom20结合相关片段的鉴定。我们通过添加大鼠或酵母Tom20的胞质受体结构域,监测了五种不同的15N标记前导序列肽的NMR信号的化学位移扰动。在这些前导序列中,受扰动的片段占据不同位置,要么靠近N端,要么在C端。自旋标记实验表明,这不是由于与Tom20结合的前导序列肽的不同取向所致。本文给出的结果将为通过系统的氨基酸替换对Tom20结合元件进行详细分析提供一个起点。

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