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Overexpression of yeast Hsp110 homolog Sse1p suppresses ydj1-151 thermosensitivity and restores Hsp90-dependent activity

机译:酵母Hsp110同源Sse1p的过表达抑制ydj1-151热敏性并恢复Hsp90依赖的活性

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摘要

The Saccharomyces cerevisiae heat-shock protein (Hsp)40, Ydj1p, is involved in a variety of cellular activities that control polypeptide fate, such as folding and translocation across intracellular membranes. To elucidate the mechanism of Ydj1p action, and to identify functional partners, we screened for multicopy suppressors of the temperature-sensitive ydj1-151 mutant and identified a yeast Hsp110, SSE1. Overexpression of Sse1p also suppressed the folding defect of v-Src kinase in the ydjl-151 mutant and partially reversed the alpha-factor translocation defect. SSE1-dependent suppression of ydjl-151 thermosensitivity required the wild-type ATP-binding domain of Sse1p. However, the Sse1p mutants maintained heat-denatured firefly luciferase in a folding-competent state in vitro and restored human androgen receptor folding in sse1 mutant cells. Because the folding of both v-Src kinase and human androgen receptor in yeast requires the Hsp90 complex, these data suggest that Ydj1p and Sse1p are interacting cochaperones in the Hsp90 complex and facilitate Hsp90-dependent activity. [References: 52]
机译:酿酒酵母热休克蛋白(Hsp)40,Ydj1p,参与控制多肽命运的多种细胞活动,例如折叠和跨细胞膜转运。为了阐明Ydj1p作用的机制并鉴定功能性伴侣,我们筛选了对温度敏感的ydj1-151突变体的多拷贝抑制剂,并鉴定了酵母Hsp110,SSE1。 Sse1p的过表达还抑制了ydjl-151突变体中v-Src激酶的折叠缺陷,并部分逆转了α因子易位缺陷。 SSE1依赖的ydjl-151热敏性抑制需要Sse1p的野生型ATP结合域。但是,Sse1p突变体在体外可折叠状态下保持热变性萤火虫荧光素酶,并在sse1突变体细胞中恢复人类雄激素受体的折叠。由于酵母中v-Src激酶和人类雄激素受体的折叠都需要Hsp90复合体,因此这些数据表明Ydj1p和Sse1p在Hsp90复合体中与伴侣伴侣相互作用并且促进了Hsp90依赖性活性。 [参考:52]

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