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Cleavage of precursors by the mitochondrial processing peptidase requires a compatible mature protein or an intermediate octapeptide

机译:通过线粒体加工肽酶裂解前体需要相容的成熟蛋白或中间八肽

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摘要

Many precursors of mitochondrial proteins are processed in two successive steps by independent matrix peptidases (MPP and MIP), whereas others are cleaved in a single step by MPP alone. To explain this dichotomy, we have constructed deletions of all or part of the octapeptide characteristic of a twice cleaved precursor (human ornithine transcarbamylase [pOTC]), have exchanged leader peptide sequences between once-cleaved (human methylmalonyl-CoA mutase [pMUT]; yeast F1ATPase beta-subunit [pF1 beta]) and twice-cleaved (pOTC; rat malate dehydrogenase (pMDH); Neurospora ubiquinol-cytochrome c reductase iron-sulfur subunit [pFe/S]) precursors, and have incubated these proteins with purified MPP and MIP. When the octapeptide of pOTC was deleted, or when the entire leader peptide of a once-cleaved precursor (pMUT or pF1 beta) was joined to the mature amino terminus of a twice-cleaved precursor (pOTC or pFe/S), no cleavage was produced by either protease. Cleavage of these constructs by MPP was restored by re- inserting as few as two amino-terminal residues of the octapeptide or of the mature amino terminus of a once-cleaved precursor. We conclude that the mature amino terminus of a twice-cleaved precursor is structurally incompatible with cleavage by MPP; such proteins have evolved octapeptides cleaved by MIP to overcome this incompatibility.
机译:线粒体蛋白的许多前体在两个连续的步骤中被独立的基质肽酶(MPP和MIP)加工,而其他的单个前体仅被MPP裂解。为了解释这种二分法,我们构建了两次裂解的前体(人鸟氨酸转氨甲酰酶[pOTC])的全部或部分八肽特征的缺失,在一次裂解的(人甲基丙二酰-CoA突变酶[pMUT])之间交换了前导肽序列。酵母F1ATPaseβ亚基[pF1β])和两次裂解的酶(pOTC;大鼠苹果酸脱氢酶(pMDH);神经孢子泛醇-细胞色素c还原酶铁-硫亚基[pFe / S])前体,并将这些蛋白与纯化的MPP一起孵育和MIP。当删除pOTC的八肽时,或一次切割的前体(pMUT或pF1 beta)的整个前导肽与两次切割的前体(pOTC或pFe / S)的成熟氨基末端连接时,则没有切割。由任何一种蛋白酶产生。通过重新插入一次裂解的前体的八肽或成熟氨基末端的少至两个氨基末端残基,可以恢复MPP对这些构建体的裂解。我们得出结论,两次裂解的前体的成熟氨基末端与MPP的裂解在结构上不相容;这样的蛋白质已经进化出被MIP切割的八肽,以克服这种不相容性。

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  • 年度 1991
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