Imai Junta, Katagiri Hideki, Yamada Tetsuya, Ishigaki Yasushi, Suzuki Toshinobu, Kudo Hirohito, Uno Kenji, Hasegawa Yutaka, Gao Junhong, Kaneko Keizo, Ishihara Hisamitsu, Niijima Akira, Nakazato Masamitsu, Asano Tomoichiro, Minokoshi Yasuhiko, Oka Yoshitomo
Division of Molecular Metabolism and Diabetes, Tohoku University Graduate School of Medicine, Sendai 980-8575, Japan.
Science. 2008 Nov 21;322(5905):1250-4. doi: 10.1126/science.1163971.
Metabolic regulation in mammals requires communication between multiple organs and tissues. The rise in the incidence of obesity and associated metabolic disorders, including type 2 diabetes, has renewed interest in interorgan communication. We used mouse models to explore the mechanism whereby obesity enhances pancreatic beta cell mass, pathophysiological compensation for insulin resistance. We found that hepatic activation of extracellular regulated kinase (ERK) signaling induced pancreatic beta cell proliferation through a neuronal-mediated relay of metabolic signals. This metabolic relay from the liver to the pancreas is involved in obesity-induced islet expansion. In mouse models of insulin-deficient diabetes, liver-selective activation of ERK signaling increased beta cell mass and normalized serum glucose levels. Thus, interorgan metabolic relay systems may serve as valuable targets in regenerative treatments for diabetes.
哺乳动物的代谢调节需要多个器官和组织之间进行通讯。肥胖及相关代谢紊乱(包括2型糖尿病)发病率的上升,重新引发了人们对器官间通讯的兴趣。我们使用小鼠模型来探究肥胖增强胰腺β细胞量(即对胰岛素抵抗的病理生理补偿)的机制。我们发现,细胞外调节激酶(ERK)信号在肝脏中的激活,通过神经元介导的代谢信号传递诱导了胰腺β细胞增殖。这种从肝脏到胰腺的代谢信号传递参与了肥胖诱导的胰岛扩张。在胰岛素缺乏型糖尿病小鼠模型中,ERK信号的肝脏选择性激活增加了β细胞量,并使血清葡萄糖水平恢复正常。因此,器官间代谢信号传递系统可能成为糖尿病再生治疗中有价值的靶点。
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