首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >A novel intermembrane space–targeting signal docks cysteines onto Mia40 during mitochondrial oxidative folding
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A novel intermembrane space–targeting signal docks cysteines onto Mia40 during mitochondrial oxidative folding

机译:在线粒体氧化折叠过程中新型的膜间空间定向信号将半胱氨酸停泊在Mia40上

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摘要

Mia40 imports Cys-containing proteins into the mitochondrial intermembrane space (IMS) by ensuring their Cys-dependent oxidative folding. In this study, we show that the specific Cys of the substrate involved in docking with Mia40 is substrate dependent, the process being guided by an IMS-targeting signal (ITS) present in Mia40 substrates. The ITS is a 9-aa internal peptide that (a) is upstream or downstream of the docking Cys, (b) is sufficient for crossing the outer membrane and for targeting nonmitochondrial proteins, (c) forms an amphipathic helix with crucial hydrophobic residues on the side of the docking Cys and dispensable charged residues on the other side, and (d) fits complementary to the substrate cleft of Mia40 via hydrophobic interactions of micromolar affinity. We rationalize the dual function of Mia40 as a receptor and an oxidase in a two step–specific mechanism: an ITS-guided sliding step orients the substrate noncovalently, followed by docking of the substrate Cys now juxtaposed to pair with the Mia40 active Cys.
机译:Mia40通过确保其Cys依赖性氧化折叠将含Cys的蛋白质导入线粒体膜间空间(IMS)。在这项研究中,我们表明参与与Mia40对接的底物的特定Cys依赖于底物,该过程由Mia40底物中存在的IMS靶向信号(ITS)指导。 ITS是一种9-aa内部肽,(a)在对接Cys的上游或下游,(b)足以穿过外膜并靶向非线粒体蛋白,(c)形成两亲螺旋,在其上具有关键的疏水残基(d)通过微摩尔亲和力的疏水相互作用与Mia40的底物缝隙互补,与对接Cys的一侧和可分配的带电残基在另一侧。我们通过两步特定的机制使Mia40作为受体和氧化酶的双重功能合理化:ITS引导的滑动步骤使底物非共价定向,然后对接现在与Mia40活性Cys并置的底物Cys。

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