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Two-way communication between SecY and SecA suggests a Brownian ratchet mechanism for protein translocation

机译:SecY和SecA之间的双向通讯表明蛋白质转运的布朗棘轮机制

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摘要

The essential process of protein secretion is achieved by the ubiquitous Sec machinery. In prokaryotes, the drive for translocation comes from ATP hydrolysis by the cytosolic motor- protein SecA, in concert with the proton motive force (PMF). However, the mechanism through which ATP hydrolysis by SecA is coupled to directional movement through SecYEG is unclear. Here, we combine all-atom molecular dynamics (MD) simulations with single molecule FRET and biochemical assays. We show that ATP binding by SecA causes opening of the SecY- channel at long range, while substrates at the SecY-channel entrance feed back to regulate nucleotide exchange by SecA. This two-way communication suggests a new, unifying 'Brownian ratchet' mechanism, whereby ATP binding and hydrolysis bias the direction of polypeptide diffusion. The model represents a solution to the problem of transporting inherently variable substrates such as polypeptides, and may underlie mechanisms of other motors that translocate proteins and nucleic acids.
机译:普遍存在的Sec机制可实现蛋白质分泌的基本过程。在原核生物中,与质子原动力(PMF)协同作用,转运的动力来自胞质运动蛋白SecA的ATP水解。但是,尚不清楚通过SecA进行的ATP水解与通过SecYEG进行的定向运动偶联的机制。在这里,我们将全原子分子动力学(MD)模拟与单分子FRET和生化分析相结合。我们表明,由SecA进行的ATP结合会导致SecY通道的长距离开放,而SecY通道入口处的底物会反馈以调节SecA的核苷酸交换。这种双向交流暗示了一种新的,统一的“布朗棘轮”机制,其中ATP结合和水解作用偏向多肽扩散的方向。该模型代表了运输固有可变底物(例如多肽)问题的解决方案,并且可能是其他易位蛋白质和核酸的马达的机制的基础。

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