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结节性硬化症复合物1/2(TSC1/TSC2)和小G蛋白Rheb对雷帕霉素靶蛋白复合物1(TORC1)和雷帕霉素靶蛋白复合物2(TORC2)的活性有不同影响。

TSC1/TSC2 and Rheb have different effects on TORC1 and TORC2 activity.

作者信息

Yang Qian, Inoki Ken, Kim Eunjung, Guan Kun-Liang

机构信息

Life Sciences Institute, University of Michigan, Ann Arbor, MI 48109, USA.

出版信息

Proc Natl Acad Sci U S A. 2006 May 2;103(18):6811-6. doi: 10.1073/pnas.0602282103. Epub 2006 Apr 20.

Abstract

Target of rapamycin (TOR) plays a central role in cell growth regulation by integrating signals from growth factors, nutrients, and cellular energy levels. TOR forms two distinct physical and functional complexes, termed TOR complex 1 (TORC1) and TOR complex 2 (TORC2). TORC1, which is sensitive to rapamycin, regulates translation and cell growth, whereas TORC2, which is insensitive to rapamycin, regulates cell morphology and cell growth. The Ras homology enriched in brain (Rheb) small GTPase is known to be a key upstream activator of TORC1, although the mechanism of Rheb in TORC1 activation remains to be determined. However, the function of Rheb in the TORC2 regulation has not been elucidated. By measuring Akt and S6K phosphorylation as a functional assay for TORC1 and -2, here, we report that dRheb has an inhibitory effect on dTORC2 activity in Drosophila S2 cells. This negative effect of dRheb on dTORC2 is possibly due to a feedback mechanism involving dTORC1 and dS6K. We also observed that Rheb does not activate TORC2 in human embryonic kidney 293 cells, although it potently stimulates TORC1. Furthermore, tuberous sclerosis complex 1 (TSC1) and TSC2, which are negative regulators of Rheb, have negative and positive effects on TORC1 and -2, respectively. Our observations suggest that TSC1/2 and Rheb have different effects on the activity of TORC1 and -2, further supporting the complexity of TOR regulation.

摘要

雷帕霉素靶蛋白(TOR)通过整合来自生长因子、营养物质和细胞能量水平的信号,在细胞生长调控中发挥核心作用。TOR形成两种不同的物理和功能复合物,分别称为TOR复合物1(TORC1)和TOR复合物2(TORC2)。对雷帕霉素敏感的TORC1调节翻译和细胞生长,而对雷帕霉素不敏感的TORC2调节细胞形态和细胞生长。富含脑的Ras同源物(Rheb)小GTP酶已知是TORC1的关键上游激活剂,尽管Rheb激活TORC1的机制仍有待确定。然而,Rheb在TORC2调节中的功能尚未阐明。通过测量Akt和S6K磷酸化作为TORC1和TORC2的功能检测,在此我们报告dRheb对果蝇S2细胞中的dTORC2活性具有抑制作用。dRheb对dTORC2的这种负面影响可能是由于涉及dTORC1和dS6K的反馈机制。我们还观察到,Rheb在人胚肾293细胞中不激活TORC2,尽管它能有效刺激TORC1。此外,作为Rheb负调节因子的结节性硬化复合物1(TSC-1)和TSC2,分别对TORC1和TORC-TORC2具有负向和正向作用。我们的观察结果表明,TSC1/2和Rheb对TORC1和TORC2的活性有不同影响,进一步支持了TOR调节的复杂性。

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