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Merck

Rheb1 promotes glucose-stimulated insulin secretion in human and mouse β-cells by upregulating GLUT expression.

Metabolism: clinical and experimental (2021-08-11)
Yan Yang, Zixin Cai, Zhenhong Pan, Fen Liu, Dandan Li, Yujiao Ji, Jiaxin Zhong, Hairong Luo, Shanbiao Hu, Lei Song, Shaojie Yu, Ting Li, Jiequn Li, Xianhua Ma, Weiping Zhang, Zhiguang Zhou, Feng Liu, Jingjing Zhang
RESUMEN

Reduced β-cell mass and impaired β-cell function are primary causes of all types of diabetes. However, the intrinsic molecular mechanism that regulates β-cell growth and function remains elusive. Here, we demonstrate that the small GTPase Rheb1 is a critical regulator of glucose-stimulated insulin secretion (GSIS) in β-cells. Rheb1 was highly expressed in mouse and human islets. In addition, β-cell-specific knockout of Rheb1 reduced the β-cell size and mass by suppressing β-cell proliferation and increasing β-cell apoptosis. However, tamoxifen-induced deletion of Rheb1 in β-cells had no significant effect on β-cell mass and size but significantly impaired GSIS. Rheb1 facilitates GSIS in human or mouse islets by upregulating GLUT1 or GLUT2 expression, respectively, in a mTORC1 signaling pathway-dependent manner. Our findings reveal a critical role of Rheb1 in regulating GSIS in β-cells and identified a new target for the therapeutic treatment of diabetes mellitus.

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Sigma-Aldrich
Estroptozocina, ≥75% α-anomer basis, ≥98% (HPLC), powder
Roche
Kit de detección de muerte celular in situ, POD, sufficient for ≤50 tests
Sigma-Aldrich
Monoclonal Anti-Insulin antibody produced in mouse, clone K36AC10, ascites fluid
Sigma-Aldrich
Anti-GLUT-2, from rabbit, purified by affinity chromatography