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UBL/BAG结构域共伴侣蛋白通过Hsf1的组成型激活在过表达时引起细胞应激。

UBL/BAG-domain co-chaperones cause cellular stress upon overexpression through constitutive activation of Hsf1.

作者信息

Poulsen Esben G, Kampmeyer Caroline, Kriegenburg Franziska, Johansen Jens V, Hofmann Kay, Holmberg Christian, Hartmann-Petersen Rasmus

机构信息

The Linderstrøm-Land Centre, Department of Biology, University of Copenhagen, Ole Maaløes Vej 5, 2200, Copenhagen N, Denmark.

Biotech Research and Innovation Centre, University of Copenhagen, Ole Maaløes Vej 5, 2200, Copenhagen N, Denmark.

出版信息

Cell Stress Chaperones. 2017 Jan;22(1):143-154. doi: 10.1007/s12192-016-0751-z. Epub 2016 Dec 14.

Abstract

As a result of exposure to stress conditions, mutations, or defects during synthesis, cellular proteins are prone to misfold. To cope with such partially denatured proteins, cells mount a regulated transcriptional response involving the Hsf1 transcription factor, which drives the synthesis of molecular chaperones and other stress-relieving proteins. Here, we show that the fission yeast Schizosaccharomyces pombe orthologues of human BAG-1, Bag101, and Bag102, are Hsp70 co-chaperones that associate with 26S proteasomes. Only a subgroup of Hsp70-type chaperones, including Ssa1, Ssa2, and Sks2, binds Bag101 and Bag102 and key residues in the Hsp70 ATPase domains, required for interaction with Bag101 and Bag102, were identified. In humans, BAG-1 overexpression is typically observed in cancers. Overexpression of bag101 and bag102 in fission yeast leads to a strong growth defect caused by triggering Hsp70 to release and activate the Hsf1 transcription factor. Accordingly, the bag101-linked growth defect is alleviated in strains containing a reduced amount of Hsf1 but aggravated in hsp70 deletion strains. In conclusion, we propose that the fission yeast UBL/BAG proteins release Hsf1 from Hsp70, leading to constitutive Hsf1 activation and growth defects.

摘要

由于在合成过程中受到应激条件、突变或缺陷的影响,细胞蛋白质容易发生错误折叠。为了应对这种部分变性的蛋白质,细胞会启动一种由热休克转录因子1(Hsf1)参与的调控转录反应,该因子驱动分子伴侣和其他应激缓解蛋白的合成。在此,我们表明人类BAG-1、Bag101和Bag102在裂殖酵母粟酒裂殖酵母中的直系同源物是与26S蛋白酶体相关的Hsp70共伴侣蛋白。只有包括Ssa1、Ssa2和Sks2在内的Hsp70型伴侣蛋白亚组能与Bag101和Bag102结合,并且确定了Hsp70 ATP酶结构域中与Bag101和Bag102相互作用所需的关键残基。在人类中,癌症中通常会观察到BAG-1的过表达。在裂殖酵母中过表达bag101和bag102会导致强烈的生长缺陷,这是由触发Hsp70释放并激活Hsf1转录因子引起的。因此,在含有较少Hsf1的菌株中,与bag101相关的生长缺陷会得到缓解,但在hsp70缺失菌株中会加剧。总之,我们提出裂殖酵母UBL/BAG蛋白从Hsp70释放Hsf1,导致Hsf1组成型激活和生长缺陷。

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