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Saccharomyces cerevisiae Rot1 Is an Essential Molecular Chaperone in the Endoplasmic Reticulum

机译:酿酒酵母Rot1是内质网中必不可少的分子伴侣。

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摘要

Molecular chaperones prevent aggregation of denatured proteins in vitro and are thought to support folding of diverse proteins in vivo. Chaperones may have some selectivity for their substrate proteins, but knowledge of particular in vivo substrates is still poor. We here show that yeast Rot1, an essential, type-I ER membrane protein functions as a chaperone. Recombinant Rot1 exhibited antiaggregation activity in vitro, which was partly impaired by a temperature-sensitive rot1-2 mutation. In vivo, the rot1-2 mutation caused accelerated degradation of five proteins in the secretory pathway via ER-associated degradation, resulting in a decrease in their cellular levels. Furthermore, we demonstrate a physical and probably transient interaction of Rot1 with four of these proteins. Collectively, these results indicate that Rot1 functions as a chaperone in vivo supporting the folding of those proteins. Their folding also requires BiP, and one of these proteins was simultaneously associated with both Rot1 and BiP, suggesting that they can cooperate to facilitate protein folding. The Rot1-dependent proteins include a soluble, type I and II, and polytopic membrane proteins, and they do not share structural similarities. In addition, their dependency on Rot1 appeared different. We therefore propose that Rot1 is a general chaperone with some substrate specificity.
机译:分子伴侣可防止变性蛋白质在体外聚集,并被认为可支持体内多种蛋白质的折叠。伴侣蛋白对其底物蛋白可能具有一定的选择性,但是对特定体内底物的了解仍然很薄。我们在这里显示酵母Rot1,一种必不可少的I型ER膜蛋白,起着分子伴侣的作用。重组Rot1在体外表现出抗聚集活性,这部分受温度敏感性rot1-2突变的影响。在体内,rot1-2突变通过ER相关降解导致分泌途径中的5种蛋白质加速降解,从而导致其细胞水平降低。此外,我们证明了Rot1与这些蛋白中的四种的物理相互作用,可能是瞬时相互作用。总体而言,这些结果表明Rot1在体内起分子伴侣的作用,支持这些蛋白质的折叠。它们的折叠还需要BiP,并且其中一种蛋白质同时与Rot1和BiP相关,这表明它们可以协同作用促进蛋白质折叠。 Rot1依赖性蛋白包括可溶的I型和II型以及多位膜蛋白,它们不具有结构相似性。另外,它们对Rot1的依赖性似乎有所不同。因此,我们建议Rot1是具有某些底物特异性的普通分子伴侣。

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