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The microRNA-29 Family Dictates the Balance Between Homeostatic and Pathological Glucose Handling in Diabetes and Obesity

机译:microRNA-29家族决定糖尿病和肥胖患者体内稳态和病理性葡萄糖处理之间的平衡

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摘要

The microRNA-29 (miR-29) family is among the most abundantly expressed microRNA in the pancreas and liver. Here, we investigated the function of miR-29 in glucose regulation using miR-29a/b-1 (miR-29a)-deficient mice and newly generated miR-29b-2/c (miR-29c)-deficient mice. We observed multiple independent functions of the miR-29 family, which can be segregated into a hierarchical physiologic regulation of glucose handling. miR-29a, and not miR-29c, was observed to be a positive regulator of insulin secretion in vivo, with dysregulation of the exocytotic machinery sensitizing β-cells to overt diabetes after unfolded protein stress. By contrast, in the liver both miR-29a and miR-29c were important negative regulators of insulin signaling via phosphatidylinositol 3-kinase regulation. Global or hepatic insufficiency of miR-29 potently inhibited obesity and prevented the onset of diet-induced insulin resistance. These results demonstrate strong regulatory functions for the miR-29 family in obesity and diabetes, culminating in a hierarchical and dose-dependent effect on premature lethality.
机译:microRNA-29(miR-29)家族是胰腺和肝脏中表达最丰富的microRNA之一。在这里,我们调查了miR-29在使用miR-29a / b-1(miR-29a)缺陷小鼠和新生成的miR-29b-2 / c(miR-29c)缺陷小鼠进行葡萄糖调节中的功能。我们观察到了miR-29家族的多种独立功能,可以将其分离为葡萄糖处理的分级生理调节。观察到miR-29a,而不是miR-29c,是体内胰岛素分泌的正调节剂,胞外机制的失调使蛋白质细胞在未受应激后使β细胞对明显的糖尿病敏感。相反,在肝脏中,miR-29a和miR-29c都是通过磷脂酰肌醇3-激酶调节胰岛素信号的重要负调节剂。 miR-29的整体或肝功能不全有效抑制了肥胖症,并阻止了饮食引起的胰岛素抵抗。这些结果表明,miR-29家族在肥胖和糖尿病中具有强大的调节功能,最终导致对过早杀伤力的分级和剂量依赖性作用。

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