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冷冻电镜结构的整个 FtsH-HflKC AAA 蛋白酶复合物。

Cryo-EM structure of the entire FtsH-HflKC AAA protease complex.

机构信息

School of Biological Sciences, Nanyang Technological University, Singapore 637551, Singapore; NTU Institute of Structural Biology, Nanyang Technological University, Singapore 639798, Singapore.

Institute for Life and Medical Sciences, Kyoto University, Kyoto 606-8507, Japan.

出版信息

Cell Rep. 2022 May 31;39(9):110890. doi: 10.1016/j.celrep.2022.110890.

Abstract

The membrane-bound AAA protease FtsH is the key player controlling protein quality in bacteria. Two single-pass membrane proteins, HflK and HflC, interact with FtsH to modulate its proteolytic activity. Here, we present structure of the entire FtsH-HflKC complex, comprising 12 copies of both HflK and HflC, all of which interact reciprocally to form a cage, as well as four FtsH hexamers with periplasmic domains and transmembrane helices enclosed inside the cage and cytoplasmic domains situated at the base of the cage. FtsH K61/D62/S63 in the β2-β3 loop in the periplasmic domain directly interact with HflK, contributing to complex formation. Pull-down and in vivo enzymatic activity assays validate the importance of the interacting interface for FtsH-HflKC complex formation. Structural comparison with the substrate-bound human m-AAA protease AFG3L2 offers implications for the HflKC cage in modulating substrate access to FtsH. Together, our findings provide a better understanding of FtsH-type AAA protease holoenzyme assembly and regulation.

摘要

膜结合的 AAA 蛋白酶 FtsH 是控制细菌蛋白质质量的关键因子。两种单次跨膜蛋白 HflK 和 HflC 与 FtsH 相互作用,调节其蛋白水解活性。在这里,我们展示了整个 FtsH-HflKC 复合物的结构,包括 12 个 HflK 和 HflC 分子,它们相互作用形成一个笼状结构,同时还有四个 FtsH 六聚体,其周质域和跨膜螺旋位于笼内,细胞质域位于笼的底部。FtsH 在周质域β2-β3 环中的 K61/D62/S63 直接与 HflK 相互作用,有助于复合物的形成。下拉和体内酶活性测定验证了相互作用界面对于 FtsH-HflKC 复合物形成的重要性。与结合底物的人 m-AAA 蛋白酶 AFG3L2 的结构比较,为 HflKC 笼调节底物进入 FtsH 提供了启示。总之,我们的研究结果为 FtsH 型 AAA 蛋白酶全酶组装和调节提供了更好的理解。

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