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An InCytes from MBC Selection: Farnesylation of Ydj1 Is Required for In Vivo Interaction with Hsp90 Client Proteins

机译:从MBC选择中获得InCytes:与Hsp90客户蛋白进行体内相互作用需要Ydj1的法尼基化

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摘要

Ydj1 of Saccharomyces cerevisiae is an abundant cytosolic Hsp40, or J-type, molecular chaperone. Ydj1 cooperates with Hsp70 of the Ssa family in the translocation of preproteins to the ER and mitochondria and in the maturation of Hsp90 client proteins. The substrate-binding domain of Ydj1 directly interacts with steroid receptors and is required for the activity of diverse Hsp90-dependent client proteins. However, the effect of Ydj1 alteration on client interaction was unknown. We analyzed the in vivo interaction of Ydj1 with the protein kinase Ste11 and the glucocorticoid receptor. Amino acid alterations in the proposed client-binding domain or zinc-binding domain had minor effects on the physical interaction of Ydj1 with both clients. However, alteration of the carboxy-terminal farnesylation signal disrupted the functional and physical interaction of Ydj1 and Hsp90 with both clients. Similar effects were observed upon deletion of RAM1, which encodes one of the subunits of yeast farnesyltransferase. Our results indicate that farnesylation is a major factor contributing to the specific requirement for Ydj1 in promoting proper regulation and activation of diverse Hsp90 clients.
机译:酿酒酵母的Ydj1是丰富的细胞质Hsp40或J型分子伴侣。 Ydj1与Ssa家族的Hsp70在前蛋白向ER和线粒体的转运以及Hsp90客户蛋白的成熟中合作。 Ydj1的底物结合域直接与类固醇受体相互作用,是各种Hsp90依赖客户蛋白的活性所必需的。但是,未知Ydj1更改对客户端交互的影响。我们分析了Ydj1与蛋白激酶Ste11和糖皮质激素受体的体内相互作用。建议的客户绑定域或锌绑定域中的氨基酸改变对Ydj1与两个客户的物理相互作用影响较小。但是,羧基端法尼基化信号的改变破坏了Ydj1和Hsp90与两个客户的功能和物理相互作用。在删除RAM1时观察到类似的效果,RAM1编码酵母法呢基转移酶的一个亚基。我们的结果表明,法尼基化是促使Ydj1促进各种Hsp90客户正确调控和激活的特定要求的主要因素。

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