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Glucose regulates the release of orexin-a from the endocrine pancreas.

机译:葡萄糖调节内分泌胰腺中orexin-a的释放。

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Orexins (hypocretins) are novel neuropeptides that appear to play a role in the regulation of energy balances. Orexin-A (OXA) increases food intake in rodents, and fasting activates OXA neurons in both the lateral hypothalamic area and gut. OXA is also found in the endocrine pancreas; however, little is known about its release or functional significance. In this study, we show that depolarizing stimuli evoke the release of OXA from rat pancreatic islets in a calcium-dependent manner. Moreover, OXA release is stimulated by low glucose (2.8 mmol/l), similar to glucagon secretion, and inhibited by high glucose (16.7 mmol/l). Fasting increases plasma OXA, supporting the idea that orexin is released in response to hypoglycemia. Cells that secrete glucagon and insulin contain OXA and both cell types express orexin receptors. OXA increases glucagon secretion and decreases glucose-stimulated insulin release from isolated islets. OXA infusion increases plasma glucagon and glucose levels and decreases plasma insulin in fasted rats. We conclude that orexin-containing islet cells, like those in the brain and gut, are glucosensitive and part of a network of glucose "sensing" cells that becomes activated when blood glucose levels fall. OXA may modulate islet hormone secretion to maintain blood glucose levels during fasting.
机译:食欲素(hypocretins)是新型的神经肽,似乎在调节能量平衡中发挥作用。 Orexin-A(OXA)增加了啮齿动物的食物摄入,禁食可激活下丘脑外侧区域和肠道的OXA神经元。在内分泌胰腺中也发现了OXA。但是,对其释放或功能意义知之甚少。在这项研究中,我们表明去极化刺激以钙依赖的方式引起大鼠胰岛中OXA的释放。此外,与胰高血糖素的分泌相似,低葡萄糖(2.8 mmol / l)刺激了OXA的释放,而高葡萄糖(16.7 mmol / l)抑制了OXA的释放。空腹会增加血浆中的OXA,从而支持食欲素释放以应对低血糖症。分泌胰高血糖素和胰岛素的细胞含有OXA,两种细胞类型都表达orexin受体。 OXA增加胰高血糖素的分泌,并减少葡萄糖刺激的胰岛素从分离的胰岛中的释放。 OXA输注会增加禁食大鼠的血浆胰高血糖素和葡萄糖水平,并降低血浆胰岛素。我们得出的结论是,含食欲素的胰岛细胞(如大脑和肠中的胰岛细胞)对葡萄糖敏感,并且是葡萄糖“传感”细胞网络的一部分,当血糖水平下降时,该细胞就会被激活。 OXA可以调节禁食期间胰岛激素的分泌,以维持血糖水平。

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