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Diminished degradation of yeast cytochrome c by interactions with its physiological partners.

机译:通过与其生理伴侣的相互作用减少酵母细胞色素c的降解。

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The level and structure of yeast iso-1-cytochrome c and iso-2-cytochrome c, encoded by the nuclear genes CYC1 and CYC7, respectively, are normally not altered in rho- mutants, which completely lack the cytochromes a.a3 subunits and cytochrome b that are encoded by mitochondrial DNA. In contrast, iso-cytochromes c containing the amino acid change Thr-78-->Ile (T78I) were observed at the normal or near-normal wild-type level in rho+ strains but were completely absent in rho- mutants. We have demonstrated with the "global" suppressor mutation Asn-52-->Ile and by pulse-chase labeling that the T78I iso-1-cytochrome c undergoes rapid cellular degradation in rho- mutants. Furthermore, specific mutations revealed that the deficiency of T78I iso-1 cytochrome c can be caused by the lack of cytochrome a.a3 or cytochrome c1, but not by the lack of cytochrome b. Thus, this and certain other, but not all, labile forms of cytochrome c are protected from degradation by the interaction with its physiological partners.
机译:分别由核基因CYC1和CYC7编码的酵母异1-细胞色素c和异2-细胞色素c的水平和结构在rho-突变体中通常不会发生改变,它们完全缺乏细胞色素a.a3亚基和线粒体DNA编码的细胞色素b。相反,在rho +菌株中观察到含有氨基酸变化Thr-78-> Ile(T78I)的异细胞色素c,但在rho-突变体中却完全缺失。我们已经通过“全局”抑制子突变Asn-52-> Ile进行了证明,并通过脉冲追踪标记证明T78I iso-1-细胞色素c在rho突变体中经历了快速的细胞降解。此外,特异性突变表明,T78I iso-1细胞色素c的缺乏可能是由于细胞色素a.a3或细胞色素c1的缺乏引起的,而不是由于细胞色素b的缺乏引起的。因此,这种和某些但不是全部不稳定形式的细胞色素c通过与其生理伴侣的相互作用而被保护免于降解。

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