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HSF1 is required for induction of mitochondrial chaperones during the mitochondrial unfolded protein response

机译:在线粒体展开蛋白应答期间,诱导线粒体伴侣需要HSF1

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The mitochondrial unfolded protein response (UPRsupmt/sup) is characterized by the transcriptional induction of mitochondrial chaperone and protease genes in response to impaired mitochondrial proteostasis and is regulated by ATF5 and CHOP in mammalian cells. However, the detailed mechanisms underlying the UPRsupmt/sup are currently unclear. Here, we show that HSF1 is required for activation of mitochondrial chaperone genes, including HSP60, HSP10, and mtHSP70, in mouse embryonic fibroblasts during inhibition of matrix chaperone TRAP1, protease Lon, or electron transfer complex 1 activity. HSF1 bound constitutively to mitochondrial chaperone gene promoters, and we observed that its occupancy was remarkably enhanced at different levels during the UPRsupmt/sup. Furthermore, HSF1 supported the maintenance of mitochondrial function under the same conditions. These results demonstrate that HSF1 is required for induction of mitochondrial chaperones during the UPRsupmt/sup, and thus, it may be one of the guardians of mitochondrial function under conditions of impaired mitochondrial proteostasis.
机译:线粒体展开蛋白响应(UPR mt )的特征在于线粒体伴侣伴蛋白质和蛋白酶基因的转录诱导,响应于受损的线粒体蛋白质蛋白质,并通过ATF5和哺乳动物细胞中的斩扣调节。但是,UPR mt 的详细机制目前不清楚。在这里,我们表明,在抑制基质伴侣Trap1,蛋白酶LOL或电子转移络合物1活性期间,在小鼠胚胎成纤维细胞中,在小鼠胚胎成纤维细胞中,在小鼠胚胎成纤维细胞中,需要HSF1。 HSF1与线粒体伴侣基因启动子组成思考,我们观察到在UPR Mt 期间,其占用显着增强。此外,HSF1支持在相同条件下维持线粒体功能。这些结果表明,在UPR mt期间诱导线粒体伴侣,因此,在受损线粒体蛋白质棘上的条件下,它可以是线粒体功能的监护人之一。

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