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Autocatalytic Processing of m-AAA Protease Subunits in Mitochondria

机译:线粒体中m-AAA蛋白酶亚基的自催化加工

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m -AAA proteases are ATP-dependent proteolytic machines in the inner membrane of mitochondria which are crucial for the maintenance of mitochondrial activities. Conserved nuclear-encoded subunits, termed paraplegin, Afg3l1, and Afg3l2, form various isoenzymes differing in their subunit composition in mammalian mitochondria. Mutations in different m -AAA protease subunits are associated with distinct neuronal disorders in human. However, the biogenesis of m -AAA protease complexes or of individual subunits is only poorly understood. Here, we have examined the processing of nuclear-encoded m -AAA protease subunits upon import into mitochondria and demonstrate autocatalytic processing of Afg3l1 and Afg3l2. The mitochondrial processing peptidase MPP generates an intermediate form of Afg3l2 that is matured autocatalytically. Afg3l1 or Afg3l2 are also required for maturation of newly imported paraplegin subunits after their cleavage by MPP. Our results establish that mammalian m -AAA proteases can act as processing enzymes in vivo and reveal overlapping activities of Afg3l1 and Afg3l2. These findings might be of relevance for the pathogenesis of neurodegenerative disorders associated with mutations in different m -AAA protease subunits.
机译:m -AAA蛋白酶是线粒体内膜中依赖ATP的蛋白水解机器,对维持线粒体活性至关重要。保守的核编码亚基,称为截瘫,Afg3l1和Afg3l2,在哺乳动物线粒体中形成不同亚基组成的各种同工酶。不同的m -AAA蛋白酶亚基的突变与人类不同的神经元疾病有关。但是,对m -AAA蛋白酶复合物或单个亚基的生物发生了解甚少。在这里,我们已经检查了导入线粒体后核编码的m -AAA蛋白酶亚基的加工,并证明了Afg3l1和Afg3l2的自动催化加工。线粒体加工肽酶MPP产生Afg3l2的中间形式,该中间形式自动催化成熟。 Ampg3l1或Afg3l2也​​是新导入的截瘫亚基被MPP切割后成熟所必需的。我们的结果证实,哺乳动物的m -AAA蛋白酶可以在体内充当加工酶,并揭示Afg3l1和Afg3l2的重叠活性。这些发现可能与与不同的m -AAA蛋白酶亚基中的突变相关的神经退行性疾病的发病机制有关。

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