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Size Motion and Function of the SecY Translocon Revealed by Molecular Dynamics Simulations with Virtual Probes

机译:通过虚拟探针的分子动力学模拟揭示了SecY转运子的大小运动和功能

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摘要

We report a hybrid, coarse-grained and atomistic, molecular dynamics simulation study of the size, motion, and function of the SecY protein-conducting channel. Growing and pushing virtual soft ball constructs through the pore of SecY, we mimic the push-through of polypeptides, performed cotranslationally by the ribosome and posttranslationally by the SecA ATPase. Forced lateral opening of a “front gate” between transmembrane helices is also induced by the passage of the virtual probes, with implications for the membrane insertion of peptides. We conclude that the SecY channel can stretch to allow passage of peptides with transversal sizes of ∼16 Å. The observed motion of a transmembrane helical “plug” controlling the closed and open states of the channel is consistent with experimental results and confirms previous hypotheses. Additionally, the “hinge” region for front gate opening is observed to be highly mobile as postulated. Both the forced dilation of a “ring” of residues at the middle of the pore and the lateral opening of the front gate are shown to induce plug displacement, but neither accomplish a full-extent motion of the plug to the back of the channel. For probes whose passage does not destroy the resilience of the SecY, both lateral exit and full translocation are observed, despite the fact that applied forces were always in the direction along the pore axis. Lateral exit is accompanied by front gate opening and slight plug displacement, whereas full translocation is accompanied by large plug displacement but no apparent lateral opening. Simulations also reveal that dilating the pore ring is a more effective way to destabilize the plug than intercalation of a cylinder-like probe at the front gate. Based on the simulations, the existence of a family of diverse open states is proposed.
机译:我们报告了SecY蛋白质传导通道的大小,运动和功能的混合,粗粒度和原子性的分子动力学模拟研究。通过SecY的孔生长并推动虚拟软球构造,我们模拟了由核糖体共翻译并由SecA ATPase进行翻译的多肽推入。跨膜螺旋之间的“前门”的强制侧向打开也由虚拟探针的通过引起,这涉及肽的膜插入。我们得出的结论是,SecY通道可以延伸以允许横向尺寸约为16Å的肽通过。观察到的控制通道关闭和打开状态的跨膜螺旋“塞子”运动与实验结果一致,并证实了先前的假设。另外,假设假定前门打开的“铰链”区域活动性很高。残余物的“环”在孔中间的强制扩张和前浇口的侧向开口均会引起塞子移位,但都无法完成塞子向通道后部的完全运动。对于其通过不会破坏SecY的回弹力的探头,尽管施加的力始终沿孔轴方向,但同时观察到了侧向出口和完全易位。侧向出口伴随着前门打开和轻微的塞子位移,而完全易位伴随着较大的塞子位移但没有明显的横向开口。模拟还显示,与在前门插入圆柱状探针相比,扩张孔环是使塞不稳定的更有效方法。基于这些模拟,提出了一个不同的开放状态族的存在。

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