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细菌前体蛋白转位酶:一种持续性酶的机制和构象动力学

Bacterial preprotein translocase: mechanism and conformational dynamics of a processive enzyme.

作者信息

Economou A

机构信息

Institute of Molecular Biology and Biotechnology-FORTH and Department of Biology, University of Crete, Iraklio-Crete, Greece.

出版信息

Mol Microbiol. 1998 Feb;27(3):511-8. doi: 10.1046/j.1365-2958.1998.00713.x.

Abstract

Preprotein translocase, the membrane transporter for secretory proteins, is a processive enzyme. It comprises the membrane proteins SecYEG(DFYajC) and the peripheral ATPase SecA, which acts as a motor subunit. Translocase subunits form dynamic complexes in the lipid bilayer and build an aqueous conduit through which preprotein substrates are transported at the expense of energy. Preproteins bind to translocase and trigger cycles of ATP binding and hydrolysis that drive a transition of SecA between two distinct conformational states. These changes are transmitted to SecG and lead to inversion of its membrane topology. SecA conformational changes promote directed migration of the polymeric substrate through the translocase, in steps of 20-30 aminoacyl residues. Translocase dissociates from the substrate only after the whole preprotein chain length has been transported to the trans side of the membrane, where it is fully released.

摘要

前体蛋白转运酶,即分泌蛋白的膜转运体,是一种进行性酶。它由膜蛋白SecYEG(DFYajC)和外周ATP酶SecA组成,SecA作为一个运动亚基。转运酶亚基在脂质双层中形成动态复合物,并构建一个水性通道,前体蛋白底物通过该通道以消耗能量的方式进行转运。前体蛋白与转运酶结合并触发ATP结合和水解循环,驱动SecA在两种不同构象状态之间转变。这些变化传递给SecG并导致其膜拓扑结构反转。SecA的构象变化促进聚合物底物以20 - 30个氨酰基残基的步长通过转运酶进行定向迁移。只有在整个前体蛋白链长度都被转运到膜的外侧并完全释放后,转运酶才会与底物解离。

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