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首页> 外文期刊>Molecular and Cellular Biology >Residues of Tim44 Involved in both Association with the Translocon of the Inner Mitochondrial Membrane and Regulation of Mitochondrial Hsp70 Tethering
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Residues of Tim44 Involved in both Association with the Translocon of the Inner Mitochondrial Membrane and Regulation of Mitochondrial Hsp70 Tethering

机译:Tim44的残留参与与内部线粒体膜的translocon关联和线粒体Hsp70束缚的调节。

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摘要

Translocation of proteins from the cytosol across the mitochondrial inner membrane is driven by the action of the import motor, which is associated with the translocon on the matrix side of the membrane. It is well established that an essential peripheral membrane protein, Tim44, tethers mitochondrial Hsp70 (mtHsp70), the core of the import motor, to the translocon. This Tim44-mtHsp70 interaction, which can be recapitulated in vitro, is destabilized by binding of mtHsp70 to a substrate polypeptide. Here we report that the N-terminal 167-amino-acid segment of mature Tim44 is sufficient for both interaction with mtHsp70 and destabilization of a Tim44-mtHsp70 complex caused by client protein binding. Amino acid alterations within a 30-amino-acid segment affected both the release of mtHsp70 upon peptide binding and the interaction of Tim44 with the translocon. Our results support the idea that Tim44 plays multiple roles in mitochondrial protein import by recruiting Ssc1 and its J protein cochaperone to the translocon and coordinating their interactions to promote efficient protein translocation in vivo.
机译:蛋白质从胞质穿过线粒体内膜的转运是由输入马达的作用驱动的,该马达与膜基质侧的转位子相关。公认的是,必需的外周膜蛋白Tim44将线粒体Hsp70(mtHsp70)(导入马达的核心)束缚在转位子上。可以在体外概括的Tim44-mtHsp70相互作用通过mtHsp70与底物多肽的结合而不稳定。在这里我们报告,成熟的Tim44的N端167个氨基酸段足以与mtHsp70相互作用和由客户端蛋白结合引起的Tim44-mtHsp70复合物的失稳。 30个氨基酸区段内的氨基酸改变影响肽结合后mtHsp70的释放以及Tim44与translocon的相互作用。我们的研究结果支持了Tim44在线粒体蛋白导入中发挥多种作用的想法,方法是将Ssc1及其J蛋白伴侣蛋白募集到translocon并协调它们之间的相互作用以促进体内有效的蛋白易位。

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