首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Mitochondrial Hsp90 is a ligand-activated molecular chaperone coupling ATP binding to dimer closure through a coiled-coil intermediate
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Mitochondrial Hsp90 is a ligand-activated molecular chaperone coupling ATP binding to dimer closure through a coiled-coil intermediate

机译:线粒体Hsp90是一种配体激活的分子伴侣其通过卷曲螺旋中间体将ATP结合至二聚体闭合

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摘要

Heat-shock protein of 90 kDa (Hsp90) is an essential molecular chaperone that adopts different 3D structures associated with distinct nucleotide states: a wide-open, V-shaped dimer in the apo state and a twisted, N-terminally closed dimer with ATP. Although the N domain is known to mediate ATP binding, how Hsp90 senses the bound nucleotide and facilitates dimer closure remains unclear. Here we present atomic structures of human mitochondrial Hsp90N (TRAP1N) and a composite model of intact TRAP1 revealing a previously unobserved coiled-coil dimer conformation that may precede dimer closure and is conserved in intact TRAP1 in solution. Our structure suggests that TRAP1 normally exists in an autoinhibited state with the ATP lid bound to the nucleotide-binding pocket. ATP binding displaces the ATP lid that signals the cis-bound ATP status to the neighboring subunit in a highly cooperative manner compatible with the coiled-coil intermediate state. We propose that TRAP1 is a ligand-activated molecular chaperone, which couples ATP binding to dramatic changes in local structure required for protein folding.
机译:90 kDa的热休克蛋白(Hsp90)是一种必需的分子伴侣,它采用与不同核苷酸状态相关的不同3D结构:apo态的宽开口V形二聚体和带有ATP的扭曲的N端封闭的二聚体。尽管已知N结构域介导ATP结合,但是尚不清楚Hsp90如何感测结合的核苷酸并促进二聚体封闭。在这里,我们介绍了人类线粒体Hsp90N(TRAP1N)的原子结构和完整TRAP1的复合模型,该模型揭示了以前未观察到的卷曲螺旋二聚体构象,该构象可能在二聚体封闭之前,并且在溶液中完整的TRAP1中是保守的。我们的结构表明,TRAP1通常以自抑制状态存在,并且ATP盖与核苷酸结合袋结合。 ATP结合以与螺旋螺旋中间状态兼容的高度协作方式取代了ATP盖,该盖以顺式结合的ATP状态向邻近的亚基发出信号。我们建议TRAP1是一个配体激活的分子伴侣,它将ATP结合与蛋白质折叠所需的局部结构的剧烈变化相结合。

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