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蛋白质导入线粒体基质的过程需要在线粒体外进行磷酸二酯键的切割才能完成。

Phosphodiester bond cleavage outside mitochondria is required for the completion of protein import into the mitochondrial matrix.

作者信息

Chen W J, Douglas M G

出版信息

Cell. 1987 Jun 5;49(5):651-8. doi: 10.1016/0092-8674(87)90541-1.

Abstract

The present studies show that hydrolysis of a phosphodiester bond, most likely ATP, is a distinct, second step required to complete import of the F1-ATPase beta-subunit into the mitochondria. This step follows a membrane potential-dependent first step. We show, using an inhibitor of adenine nucleotide transport and the analogue beta,gamma-AMP-PCP, that the activity required for this phosphodiester hydrolysis-dependent completion of protein import resides outside the mitochondrial inner membrane. This activity is proposed to act on the precursor at the site of translocation either to render it competent or to catalyze its vectorial movement directly through the import apparatus. This activity shares properties ascribed to proteins of the heat-shock family, which are proposed to participate in the ATP-dependent refolding of partially denatured proteins and nascent peptides.

摘要

目前的研究表明,磷酸二酯键(很可能是ATP)的水解是F1 - ATP酶β亚基完整导入线粒体所需的一个独特的第二步。这一步骤紧随膜电位依赖的第一步之后。我们使用腺嘌呤核苷酸转运抑制剂和类似物β,γ - AMP - PCP表明,这种依赖磷酸二酯水解的蛋白质导入完成所需的活性存在于线粒体内膜之外。这种活性被认为作用于转运位点的前体,要么使其具备能力,要么直接催化其通过导入装置的定向移动。这种活性具有热休克家族蛋白质的特性,热休克家族蛋白质被认为参与部分变性蛋白质和新生肽的ATP依赖重折叠。

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