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伴侣蛋白Hap46/BAG-1M和Hap50/BAG-1L及其亚型的活性

Activities of the cochaperones Hap46/BAG-1M and Hap50/BAG-1L and isoforms.

作者信息

Gehring Ulrich

机构信息

Universität Heidelberg, Percent Molekulare Evolution and Genomik, Im Neuenheimer Feld 230, D-69120 Heidelberg.

出版信息

Cell Stress Chaperones. 2006 Winter;11(4):295-303. doi: 10.1379/1466-1268(2006)11[295:aotcba]2.0.co;2.

Abstract

Since their discovery about a decade ago, human Hap46/BAG-1M, the larger isoform Hap50/BAG-1L, and related structures have caused quite some astonishment because of the seemingly unlimited array of possible interaction partners belonging to completely unrelated protein families. This problem was partially resolved when it was realized that molecular chaperones of the heat shock protein family Hsp70 are major primary association partners, which in turn, are able to bind a wide variety of unrelated protein structures, thus forming ternary complexes. Moreover, the protein folding activity of Hsp70 chaperones is affected; hence, the designation "cochaperones." Although many different proteins require mediation by Hsp70 chaperones for interactions with Hap50/BAG-1L, Hap46/BAG-1M, and isoforms, several other partner proteins are able to associate directly. In addition, Hap46/BAG-1M and Hap50/BAG-1L are also able to interact with DNA by making use of a positively charged region close to the amino terminal end of the polypeptide chain. This is the molecular basis for their effects on transcriptional activities, which are emphasized in this review and for which a molecular model is presented.

摘要

大约十年前人类Hap46/BAG-1M、较大的异构体Hap50/BAG-1L及相关结构被发现以来,因其似乎能与完全不相关蛋白质家族的无数潜在相互作用伙伴相结合,引起了不少轰动。当认识到热休克蛋白家族Hsp70的分子伴侣是主要的初始结合伙伴,而这些分子伴侣又能结合多种不相关的蛋白质结构从而形成三元复合物时,这个问题得到了部分解决。此外,Hsp70分子伴侣的蛋白质折叠活性也受到影响,因此被称为“共分子伴侣”。尽管许多不同蛋白质需要Hsp70分子伴侣介导才能与Hap50/BAG-1L、Hap46/BAG-1M及其异构体相互作用,但其他一些伙伴蛋白也能直接结合。此外,Hap46/BAG-1M和Hap50/BAG-1L还能利用多肽链氨基末端附近的带正电区域与DNA相互作用。这是它们对转录活性产生影响的分子基础,本综述对此进行了重点阐述并给出了分子模型。

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