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胰腺内质网中的热休克蛋白70分子伴侣网络——一种定量方法

The heat shock protein 70 molecular chaperone network in the pancreatic endoplasmic reticulum - a quantitative approach.

作者信息

Weitzmann Andreas, Baldes Christiane, Dudek Johanna, Zimmermann Richard

机构信息

Medizinische Biochemie und Molekularbiologie, Universität des Saarlandes, Homburg, Germany.

出版信息

FEBS J. 2007 Oct;274(19):5175-87. doi: 10.1111/j.1742-4658.2007.06039.x. Epub 2007 Sep 10.

Abstract

Traditionally, the canine pancreatic endoplasmic reticulum (ER) has been the workhorse for cell-free studies on protein transport into the mammalian ER. These studies have revealed multiple roles for the major ER-luminal heat shock protein (Hsp) 70, IgG heavy chain-binding protein (BiP), at least one of which also involves the second ER-luminal Hsp70, glucose-regulated protein (Grp) 170. In addition, at least one of these BiP activities depends on Hsp40. Up to now, five Hsp40s and two nucleotide exchange factors, Sil1 and Grp170, have been identified in the ER of different mammalian cell types. Here we quantified the various proteins of this chaperone network in canine pancreatic rough microsomes. We also characterized the various purified proteins with respect to their affinities for BiP and their effect on the ATPase activity of BiP. The results identify Grp170 as the major nucleotide exchange factor for BiP, and the resident ER-membrane proteins ER-resident J-domain protein 1 plus ER-resident J-domain protein 2/Sec63 as prime candidates for cochaperones of BiP in protein transport in the pancreatic ER. Thus, these data represent a comprehensive analysis of the BiP chaperone network that was recently linked to two human inherited diseases, polycystic liver disease and Marinesco-Sjögren syndrome.

摘要

传统上,犬胰腺内质网(ER)一直是用于蛋白质转运至哺乳动物内质网的无细胞研究的主力。这些研究揭示了内质网腔主要热休克蛋白(Hsp)70、免疫球蛋白重链结合蛋白(BiP)的多种作用,其中至少一种作用还涉及第二种内质网腔Hsp70,即葡萄糖调节蛋白(Grp)170。此外,这些BiP活性中至少有一种依赖于Hsp40。到目前为止,已在不同哺乳动物细胞类型的内质网中鉴定出五种Hsp40和两种核苷酸交换因子,即Sil1和Grp170。在此,我们对犬胰腺粗面微粒体中该伴侣蛋白网络的各种蛋白质进行了定量分析。我们还对各种纯化蛋白与BiP的亲和力及其对BiP ATP酶活性的影响进行了表征。结果确定Grp170是BiP的主要核苷酸交换因子,内质网驻留J结构域蛋白1加上内质网驻留J结构域蛋白2/ Sec63作为胰腺内质网蛋白质转运中BiP共伴侣蛋白的主要候选者。因此,这些数据代表了对最近与两种人类遗传性疾病,即多囊肝病和 Marinesco-Sjögren综合征相关的BiP伴侣蛋白网络的全面分析。

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