microRNA-205-5p is a modulator of insulin sensitivity that inhibits FOXO function

microRNA-205-5p 是一种胰岛素敏感性调节剂，可抑制 FOXO 功能

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作者：Fanny Langlet, Marcel Tarbier, Rebecca A Haeusler, Stefania Camastra, Eleuterio Ferrannini, Marc R Friedländer, Domenico Accili

期刊：

Molecular Metabolism

影响因子：

7.000

时间：

2018

起止号：

2018 Nov:17:49-60.

doi：

10.1016/j.molmet.2018.08.003

研究方向：

信号转导

Conclusions

These findings reveal a homeostatic miRNA loop regulating insulin signaling, with potential implications for in vivo glucose metabolism.

Methods

To address this question, we obtained expression profiles of FOXO-regulated murine hepatic microRNAs (miRNAs) during fasting and refeeding using mice lacking Foxo1, 3a, and 4 in liver (L-Foxo1,3a, 4).

Results

Out of 439 miRNA analyzed, 175 were differentially expressed in Foxo knockouts. Their functions were associated with insulin, Wnt, Mapk signaling, and aging. Among them, we report a striking increase of miR-205-5p expression in L-Foxo1,3a,4 knockouts, as well as in obese mice. We show that miR-205-5p gain-of-function increases AKT phosphorylation and decreases SHIP2 in primary hepatocytes, resulting in FOXO inhibition. This results in decreased hepatocyte glucose production. Consistent with these observations, miR-205-5p gain-of-function in mice lowered glucose levels and improved pyruvate tolerance. Conclusions: These findings reveal a homeostatic miRNA loop regulating insulin signaling, with potential implications for in vivo glucose metabolism.

microRNA-205-5p is a modulator of insulin sensitivity that inhibits FOXO function

microRNA-205-5p 是一种胰岛素敏感性调节剂，可抑制 FOXO 功能

Conclusions

Methods

Results

特别声明