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Inhibition of gastric inhibitory polypeptide signaling prevents obesity
Authors:Miyawaki Kazumasa  Yamada Yuichiro  Ban Nobuhiro  Ihara Yu  Tsukiyama Katsushi  Zhou Heying  Fujimoto Shimpei  Oku Akira  Tsuda Kinsuke  Toyokuni Shinya  Hiai Hiroshi  Mizunoya Wataru  Fushiki Tohru  Holst Jens Juul  Makino Mitsuhiro  Tashita Akira  Kobara Yukari  Tsubamoto Yoshiharu  Jinnouchi Takayoshi  Jomori Takahito  Seino Yutaka
Institution:Department of Diabetes and Clinical Nutrition, Graduate School of Medicine, Kyoto University, Kyoto, Japan.
Abstract:Secretion of gastric inhibitory polypeptide (GIP), a duodenal hormone, is primarily induced by absorption of ingested fat. Here we describe a novel pathway of obesity promotion via GIP. Wild-type mice fed a high-fat diet exhibited both hypersecretion of GIP and extreme visceral and subcutaneous fat deposition with insulin resistance. In contrast, mice lacking the GIP receptor (Gipr(-/-)) fed a high-fat diet were clearly protected from both the obesity and the insulin resistance. Moreover, double-homozygous mice (Gipr(-/-), Lep(ob)/Lep(ob)) generated by crossbreeding Gipr(-/-) and obese ob/ob (Lep(ob)/Lep(ob)) mice gained less weight and had lower adiposity than Lep(ob)/Lep(ob) mice. The Gipr(-/-) mice had a lower respiratory quotient and used fat as the preferred energy substrate, and were thus resistant to obesity. Therefore, GIP directly links overnutrition to obesity and it is a potential target for anti-obesity drugs.
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