Life Sciences Institute, University of Michigan, 210 Washtenaw Avenue, Ann Arbor, MI 48109-2216, USA.
Life Sciences Institute, University of Michigan, 210 Washtenaw Avenue, Ann Arbor, MI 48109-2216, USA; Department of Biochemistry, Kanazawa Medical University School of Medicine, 1-1 Daigaku, Uchinada, Kahoku-gun, Ishikawa 920-0293, Japan.
Mol Cell. 2020 Nov 5;80(3):437-451.e6. doi: 10.1016/j.molcel.2020.10.004.
Amino-acid-induced lysosomal mechanistic target of rapamycin complex 1 (mTORC1) localization through the Rag GTPases is a critical step for its activation by Rheb GTPase. However, how the mTORC1 interacts with Rheb on the lysosome remains elusive. We report that amino acids enhance the polyubiquitination of Rheb (Ub-Rheb), which shows a strong binding preference for mTORC1 and supports its activation, while the Ub-Rheb is subjected to subsequent degradation. Mechanistically, we identified ATXN3 as a Ub-Rheb deubiquitinase whose lysosomal localization is blocked by active Rag heterodimer in response to amino acid stimulation. Consistently, cells lacking functional Rag heterodimer on the lysosome accumulate Ub-Rheb, and blockade of its degradation instigates robust lysosomal mTORC1 localization and its activation without the Ragulator-Rag system. Thus, polyubiquitination of Rheb is an important post-translational modification, which facilitates the binding of mTORC1 to Rheb on the lysosome and is another crosstalk between the amino acid and growth factor signaling for mTORC1 activation.
氨基酸诱导的溶酶体雷帕霉素机制靶蛋白 1(mTORC1)通过 Rag GTPase 定位是其被 Rheb GTPase 激活的关键步骤。然而,mTORC1 如何与溶酶体上的 Rheb 相互作用仍然难以捉摸。我们报告说,氨基酸增强了 Rheb 的多泛素化(Ub-Rheb),Ub-Rheb 对 mTORC1 具有强烈的结合偏好,并支持其激活,而 Ub-Rheb 随后会被降解。在机制上,我们鉴定出 ATXN3 是一种 Ub-Rheb 的去泛素化酶,其在溶酶体上的定位被活性 Rag 异源二聚体阻断,以响应氨基酸刺激。一致地,在溶酶体上缺乏功能性 Rag 异源二聚体的细胞会积累 Ub-Rheb,并且抑制其降解会引发强大的溶酶体 mTORC1 定位及其激活,而无需 Ragulator-Rag 系统。因此,Rheb 的多泛素化是一种重要的翻译后修饰,它促进了 mTORC1 与溶酶体上 Rheb 的结合,是氨基酸和生长因子信号之间促进 mTORC1 激活的另一种相互作用。
