Integrating GHS into the Ghrelin System.

International Journal of Peptides Pub Date : 2010-01-01 Epub Date: 2010-03-18 DOI:10.1155/2010/879503
Johannes D Veldhuis, Cyril Y Bowers
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Abstract

Oligopeptide derivatives of metenkephalin were found to stimulate growth-hormone (GH) release directly by pituitary somatotrope cells in vitro in 1977. Members of this class of peptides and nonpeptidyl mimetics are referred to as GH secretagogues (GHSs). A specific guanosine triphosphatate-binding protein-associated heptahelical transmembrane receptor for GHS was cloned in 1996. An endogenous ligand for the GHS receptor, acylghrelin, was identified in 1999. Expression of ghrelin and homonymous receptor occurs in the brain, pituitary gland, stomach, endothelium/vascular smooth muscle, pancreas, placenta, intestine, heart, bone, and other tissues. Principal actions of this peptidergic system include stimulation of GH release via combined hypothalamopituitary mechanisms, orexigenesis (appetitive enhancement), insulinostasis (inhibition of insulin secretion), cardiovascular effects (decreased mean arterial pressure and vasodilation), stimulation of gastric motility and acid secretion, adipogenesis with repression of fat oxidation, and antiapoptosis (antagonism of endothelial, neuronal, and cardiomyocyte death). The array of known and proposed interactions of ghrelin with key metabolic signals makes ghrelin and its receptor prime targets for drug development.

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将 GHS 纳入胃泌素系统。
1977 年,人们发现美岑脑素的寡肽衍生物可直接刺激垂体体细胞在体外释放生长激素(GH)。这类肽类和非肽类模拟物被称为 GH 促泌剂(GHSs)。1996 年,人们克隆出了 GHS 的特异性三磷酸鸟苷结合蛋白相关七螺旋跨膜受体。GHS 受体的内源性配体酰胃泌素于 1999 年被发现。胃泌素和同名受体在大脑、垂体、胃、内皮细胞/血管平滑肌、胰腺、胎盘、肠道、心脏、骨骼和其他组织中均有表达。这种肽能系统的主要作用包括通过下丘脑-垂体联合机制刺激 GH 释放、促食欲(食欲增强)、胰岛素停滞(抑制胰岛素分泌)、心血管效应(降低平均动脉压和扩张血管)、刺激胃蠕动和胃酸分泌、抑制脂肪氧化的脂肪生成以及抗细胞凋亡(拮抗内皮细胞、神经细胞和心肌细胞死亡)。胃泌素与关键代谢信号之间的一系列已知和拟议的相互作用使胃泌素及其受体成为药物开发的首要目标。
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