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线粒体蛋白导入:机制、组分与能量学

Mitochondrial protein import: mechanisms, components and energetics.

作者信息

Schwarz E, Neupert W

机构信息

Institut für Physiologische Chemie, Universität München, Germany.

出版信息

Biochim Biophys Acta. 1994 Aug 30;1187(2):270-4. doi: 10.1016/0005-2728(94)90125-2.

Abstract

The transport of nuclear-encoded proteins from the cytosol into mitochondria is mediated by targeting (signal) sequences present on precursor forms. Most precursors of the mitochondrial matrix possess amino-terminal signals which characteristically contain hydroxylated and basic amino acids and lack acidic residues. With a minority of precursor proteins, internal sequence motifs can direct proteins to the mitochondria (Pfanner, N., Hoeben, P., Tropschug, M. and Neupert, W. (1987) J. Biol. Chem. 262, 14851-14854). The presence of a mitochondrial targeting sequence alone, however, is not sufficient for specific targeting to the organelle and further to the various subcompartments. There is the need for components which recognise the targeting sequences and others which keep the precursor protein in a translocation-competent form. Beyond the recognition step, components are required which mediate translocation across the mitochondrial membranes. Mitochondria posses two translocation machineries, one in the outer membrane and one in the inner membrane. The matrix space harbors a number of factors which participate in the import of proteins, in their unfolding and folding. Energy is required at several steps of these processes.

摘要

核编码蛋白从细胞质转运到线粒体是由前体形式上存在的靶向(信号)序列介导的。线粒体基质的大多数前体具有氨基末端信号,其特征是含有羟基化和碱性氨基酸且缺乏酸性残基。少数前体蛋白的内部序列基序可将蛋白导向线粒体(Pfanner, N., Hoeben, P., Tropschug, M.和Neupert, W. (1987) J. Biol. Chem. 262, 14851 - 14854)。然而,仅存在线粒体靶向序列不足以将其特异性靶向到该细胞器以及进一步靶向到各个亚区室。需要有识别靶向序列的组分以及使前体蛋白保持可转运形式的其他组分。除了识别步骤外,还需要介导蛋白穿过线粒体膜转运的组分。线粒体有两个转运机制,一个位于外膜,一个位于内膜。基质空间含有许多参与蛋白导入、其解折叠和折叠的因子。这些过程的几个步骤都需要能量。

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