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TORC1 决定 Fab1 脂质激酶在信号转导内体和液泡中的功能。

TORC1 Determines Fab1 Lipid Kinase Function at Signaling Endosomes and Vacuoles.

机构信息

Department of Biology/Chemistry, Biochemistry Section, University of Osnabrück, Barbarastrasse 13, 49076 Osnabrück, Germany.

Department of Biology, University of Fribourg, Chemin du Musée, CH-1700 Fribourg, Switzerland.

出版信息

Curr Biol. 2021 Jan 25;31(2):297-309.e8. doi: 10.1016/j.cub.2020.10.026. Epub 2020 Nov 5.

Abstract

Organelles of the endomembrane system maintain their identity and integrity during growth or stress conditions by homeostatic mechanisms that regulate membrane flux and biogenesis. At lysosomes and endosomes, the Fab1 lipid kinase complex and the nutrient-regulated target of rapamycin complex 1 (TORC1) control the integrity of the endolysosomal homeostasis and cellular metabolism. Both complexes are functionally connected as Fab1-dependent generation of PI(3,5)P supports TORC1 activity. Here, we identify Fab1 as a target of TORC1 on signaling endosomes, which are distinct from multivesicular bodies, and provide mechanistic insight into their crosstalk. Accordingly, TORC1 can phosphorylate Fab1 proximal to its PI3P-interacting FYVE domain, which causes Fab1 to shift to signaling endosomes, where it generates PI(3,5)P. This, in turn, regulates (1) vacuole morphology, (2) recruitment of TORC1 and the TORC1-regulatory Rag GTPase-containing EGO complex to signaling endosomes, and (3) TORC1 activity. Thus, our study unravels a regulatory feedback loop between TORC1 and the Fab1 complex that controls signaling at endolysosomes.

摘要

内质网系统的细胞器通过调节膜通量和生物发生的稳态机制,在生长或应激条件下保持其身份和完整性。在溶酶体和内体中,Fab1 脂质激酶复合物和营养调节的雷帕霉素靶蛋白复合物 1(TORC1)控制内溶酶体稳态和细胞代谢的完整性。这两个复合物在功能上是相互连接的,因为 Fab1 依赖性的 PI(3,5)P 的产生支持 TORC1 的活性。在这里,我们确定 Fab1 是信号内体上 TORC1 的靶标,信号内体与多泡体不同,并提供了它们相互作用的机制见解。因此,TORC1 可以在其与 PI3P 相互作用的 FYVE 结构域附近磷酸化 Fab1,导致 Fab1 转移到信号内体,在那里它产生 PI(3,5)P。这反过来又调节(1)液泡形态,(2)TORC1 和包含 TORC1 调节 Rag GTPase 的 EGO 复合物到信号内体的募集,以及(3)TORC1 活性。因此,我们的研究揭示了 TORC1 和 Fab1 复合物之间控制内溶酶体信号的调节反馈环。

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