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首页> 外文期刊>Current Protein and Peptide Science >Interaction between Gastric and Upper Small Intestinal Hormones in the Regulation of Hunger and Satiety: Ghrelin and Cholecystokinin Take the Central Stage
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Interaction between Gastric and Upper Small Intestinal Hormones in the Regulation of Hunger and Satiety: Ghrelin and Cholecystokinin Take the Central Stage

机译:胃和上小肠激素之间的相互作用在饥饿和饱腹感的调节中:Ghrelin和胆囊收缩素处于中心地位

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摘要

Several peptides are produced and released from endocrine cells scattered within the gastric oxyntic and the small intestinal mucosa. These peptide hormones are crucially involved in the regulation of gastrointestinal functions and food intake by conveying their information to central regulatory sites located in the brainstem as well as in the forebrain, such as hypothalamic nuclei. So far, ghrelin is the only known hormone that is peripherally produced in gastric X/A-like cells and centrally acting to stimulate food intake, whereas the suppression of feeding seems to be much more redundantly controlled by a number of gut peptides. Cholecystokinin produced in the duodenum is a well established anorexigenic hormone that interacts with ghrelin to modulate food intake indicating a regulatory network located at the first site of contact with nutrients in the stomach and upper small intestine. In addition, a number of peptides including leptin, urocortin 2, amylin and glucagon-like peptide 1 interact synergistically with CCK to potentiate its satiety signaling effect. New developments have led to the identification of additional peptides in X/A-like cells either derived from the pro-ghrelin gene by alternative splicing and posttranslational processing (obestatin) or a distinct gene (nucleobindin2esfatin-1) which have been investigated for their influence on food intake.
机译:从散布在胃氧化性和小肠粘膜中的内分泌细胞产生并释放出几种肽。这些肽激素通过将其信息传递至位于脑干以及前脑的中央调节位点(例如下丘脑核),从而至关重要地参与了胃肠功能和食物摄入的调节。到目前为止,生长素释放肽是唯一已知的在胃X / A样细胞外围产生的激素,并起着刺激食物摄取的中心作用,而进食的抑制似乎是由许多肠肽来冗余控制的。十二指肠中产生的胆囊收缩素是一种公认​​的厌食激素,可与ghrelin相互作用以调节食物摄入,这表明调节网络位于与胃和上部小肠中营养物质接触的第一个位置。另外,包括瘦蛋白,尿皮质素2,胰岛淀粉样多肽和胰高血糖素样肽1在内的许多肽与CCK协同相互作用,以增强其饱腹感信号的作用。新进展已导致在X / A样细胞中鉴定其他肽,这些肽是通过替代剪接和翻译后加工(obestatin)或前体基因(nucleobindin2 / nesfatin-1)衍生而来的,ghrulin原基因是通过选择性剪接和翻译后加工得到的。它们对食物摄入的影响。

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