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Susana Ros Delia Zafra Jordi Valles-Ortega Mar García-Rocha Stephen Forrow Jorge Domínguez Joaquim Calbó Joan J. Guinovart 《The Journal of biological chemistry》2010,285(48):37170-37177
In this study, we tested the efficacy of increasing liver glycogen synthase to improve blood glucose homeostasis. The overexpression of wild-type liver glycogen synthase in rats had no effect on blood glucose homeostasis in either the fed or the fasted state. In contrast, the expression of a constitutively active mutant form of the enzyme caused a significant lowering of blood glucose in the former but not the latter state. Moreover, it markedly enhanced the clearance of blood glucose when fasted rats were challenged with a glucose load. Hepatic glycogen stores in rats overexpressing the activated mutant form of liver glycogen synthase were enhanced in the fed state and in response to an oral glucose load but showed a net decline during fasting. In order to test whether these effects were maintained during long term activation of liver glycogen synthase, we generated liver-specific transgenic mice expressing the constitutively active LGS form. These mice also showed an enhanced capacity to store glycogen in the fed state and an improved glucose tolerance when challenged with a glucose load. Thus, we conclude that the activation of liver glycogen synthase improves glucose tolerance in the fed state without compromising glycogenolysis in the postabsorptive state. On the basis of these findings, we propose that the activation of liver glycogen synthase may provide a potential strategy for improvement of glucose tolerance in the postprandial state. 相似文献
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Julie Turnbull Erica Tiberia Sandra Pereira Xiaochu Zhao Nela Pencea Anne L. Wheeler Wen Qin Yu Alexander Ivovic Taline Naranian Nyrie Israelian Arman Draginov Mark Piliguian Paul W. Frankland Peixiang Wang Cameron A. Ackerley Adria Giacca Berge A. Minassian 《The Journal of biological chemistry》2013,288(48):34627-34637
Glycogen synthesis is a major component of the insulin response, and defective glycogen synthesis is a major portion of insulin resistance. Insulin regulates glycogen synthase (GS) through incompletely defined pathways that activate the enzyme through dephosphorylation and, more potently, allosteric activation. We identify Epm2aip1 as a GS-associated protein. We show that the absence of Epm2aip1 in mice impairs allosteric activation of GS by glucose 6-phosphate, decreases hepatic glycogen synthesis, increases liver fat, causes hepatic insulin resistance, and protects against age-related obesity. Our work identifies a novel GS-associated GS activity-modulating component of insulin resistance. 相似文献
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Xiwen Xiong Rongya Tao Ronald A. DePinho X. Charlie Dong 《The Journal of biological chemistry》2012,287(46):39107-39114
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Yao D. Cai Yongbo Xue Cindy C. Truong Jose Del Carmen-Li Christopher Ochoa Jens T. Vanselow Katherine A. Murphy Ying H. Li Xianhui Liu Ben L. Kunimoto Haiyan Zheng Caifeng Zhao Yong Zhang Andreas Schlosser Joanna C. Chiu 《Current biology : CB》2021,31(3):502-514.e7
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