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热休克蛋白90(Hsp90)辅助伴侣蛋白Sti1(p60)的体内分析

In vivo analysis of the Hsp90 cochaperone Sti1 (p60).

作者信息

Chang H C, Nathan D F, Lindquist S

机构信息

Howard Hughes Medical Institute, University of Chicago, Illinois 60637, USA.

出版信息

Mol Cell Biol. 1997 Jan;17(1):318-25. doi: 10.1128/MCB.17.1.318.

Abstract

Hsp90 interacts with Sti1 (p60) in lysates of yeast and vertebrate cells. Here we provide the first analysis of their interaction in vivo. Saccharomyces cerevisiae mutations that eliminate Sti1 or reduce intracellular concentrations of Hsp90 individually have little or no effect on growth at normal temperatures. However, when combined, the mutations greatly reduce or eliminate growth. Furthermore, overexpression of Sti1 has allele-specific effects on cells carrying various hsp90ts point mutations. These genetic interactions provide strong evidence that Hsp90 and Sti1 interact in vivo and that their functions are closely allied. Indeed, deletion of STI1 reduces the in vivo activity of the Hsp90 target protein, glucocorticoid receptor (GR). Mutations in GR that eliminate interaction with Hsp90 also eliminate the effects of the sti1 deletion. Examination of GR protein complexes in the sti1 deletion mutant reveals a selective increase in the concentration of GR-Ydj1 complexes, supporting previous hypotheses that Ydj1 functions at an early step in the maturation of GR and that Sti1 acts at an intermediate step. Deletion of STI1 also reduces the in vivo activity of another, unrelated Hsp90 target protein, v-Src. Our data indicate that Sti1 is a general factor in the maturation of Hsp90 target proteins and support earlier suggestions that Hsp90 matures even very different target proteins by a similar mechanism.

摘要

Hsp90在酵母和脊椎动物细胞裂解物中与Sti1(p60)相互作用。在此,我们首次对它们在体内的相互作用进行了分析。单独消除Sti1或降低Hsp90细胞内浓度的酿酒酵母突变对正常温度下的生长几乎没有影响。然而,当这些突变组合时,会极大地降低或消除生长。此外,Sti1的过表达对携带各种hsp90ts点突变的细胞具有等位基因特异性影响。这些遗传相互作用提供了强有力的证据,表明Hsp90和Sti1在体内相互作用,且它们的功能紧密相关。事实上,STI1的缺失会降低Hsp90靶蛋白糖皮质激素受体(GR)的体内活性。GR中消除与Hsp90相互作用的突变也消除了sti1缺失的影响。对sti1缺失突变体中GR蛋白复合物的检测显示,GR-Ydj1复合物的浓度选择性增加,支持了之前的假设,即Ydj1在GR成熟的早期阶段发挥作用,而Sti1在中间阶段发挥作用。STI1的缺失也降低了另一种不相关的Hsp90靶蛋白v-Src的体内活性。我们的数据表明,Sti1是Hsp90靶蛋白成熟的一个普遍因素,并支持了早期的观点,即Hsp90通过类似的机制使即使非常不同的靶蛋白成熟。

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