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The signal peptide plus a cluster of positive charges in prion protein dictate chaperone-mediated Sec61 channel gating

机译:信号肽加上病毒蛋白中的正电荷簇决定了分子伴侣介导的Sec61通道门控

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The Sec61-complex as a dynamic polypeptide-conducting channel mediates protein transport into the human endoplasmic reticulum (ER) with the help of additional components. ER membrane resident Hsp40-type co-chaperone Sec63 as well as the ER lumenal Hsp70-type chaperone BiP were proposed to facilitate channel opening in a precursor-specific fashion. Here, we report on their rules of engagement in ER import of the prion protein (PrP) by addressing sixteen PrP-related variants which differ in their signal peptides and mature parts, respectively. Transport into the ER of semi-permeabilized human cells was analyzed upon depletion of the components by siRNA- or toxin-treatment. The results are consistent with the view of separate functions of BiP and Sec63 and strongly suggest that the co-chaperone/chaperone-pair facilitates Sec61 channel gating to the open state when precursor polypeptides with weak signal peptides in combination with detrimental features in the adjacent mature part were targeted. Thus, we expand the view of chaperone-mediated Sec61 channel gating by providing a novel example of a polybasic motif that interferes with signal peptide-mediated Sec61 channel gating.This article has an associated First Person interview with the first author of the paper.
机译:Sec61复合体作为动态的多肽传导通道,可借助其他组件介导蛋白质转运到人内质网(ER)中。 ER膜驻留Hsp40型伴侣蛋白Sec63以及ER腔Hsp70型伴侣蛋白BiP被提议以前体特异性方式促进通道开放。在这里,我们通过研究十六种与PrP相关的变异体(其信号肽和成熟部分分别不同)来报告它们参与ER导入import病毒蛋白(PrP)的规则。在通过siRNA或毒素处理耗尽组分后,分析了半透化人细胞向ER的转运。结果与BiP和Sec63各自功能的观点一致,并强烈表明当具有弱信号肽的前体多肽与邻近成熟中的有害特征结合时,co-伴侣/伴侣对有助于Sec61通道门控打开状态部分目标。因此,我们提供了一个新的干扰信号肽介导的Sec61通道门控的多元基序实例,从而扩展了伴侣蛋白介导的Sec61通道门控的观点。

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