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胃饥饿素在能量平衡和体重稳态中的作用。

Effects of ghrelin in energy balance and body weight homeostasis.

作者信息

Mihalache Laura, Gherasim Andreea, Niţă Otilia, Ungureanu Maria Christina, Pădureanu Sergiu Serghei, Gavril Radu Sebastian, Arhire Lidia Iuliana

机构信息

Department of Internal Medicine, "Grigore T. Popa" University of Medicine and Pharmacy, Iassy, Romania.

Department of Surgery, "Grigore T. Popa" University of Medicine and Pharmacy, Iossy, Romania.

出版信息

Hormones (Athens). 2016 Feb;15(2):186-196. doi: 10.14310/horm.2002.1672.

Abstract

Ghrelin is a gut peptide composed of 28 amino acids mostly secreted in the gastric fundus mucosa. It was isolated and described in 1999 by Kojima et al. and only three years later its specific receptor, GHSR1a, was also identified. Ghrelin, the endogenous ligand for the GH secretagogue receptor, is the only peripheral orexigenic hormone that activates the receptors to be found especially in the appetite center (hypothalamus and pituitary gland). Ghrelin is present in human plasma in two forms: an inactive form known as deacylated ghrelin, and an active form called acylated ghrelin synthesized under the action of ghrelin O-acyltransferase enzyme (GOAT). The literature even mentions an extremely complex ghrelin/GOAT/GHSR system involved in the regulation of human energy, metabolism and adaptation of energy homeostasis to environmental changes. In humans, there is a preprandial rise and a postprandial fall in plasma ghrelin levels, which strongly suggest that the peptide plays a physiological role in meal initiation and may be employed in determining the amount and quality of ingested food. Besides the stimulation of food intake, ghrelin determines a decrease in energy expenditure and promotes the storage of fatty acids in adipocytes. Thus, in the human body ghrelin induces a positive energy balance, an increased adiposity gain, as well as an increase in caloric storage, seen as an adaptive mechanism to caloric restriction conditions. In the current world context, when we are witnessing an increasing availability of food and a reduction of energy expenditure to a minimum level, these mechanisms have become pathogenic. As a consequence, the hypothesis that ghrelin is involved in the current obesity epidemic has been embraced by many scholars and researchers.

摘要

胃饥饿素是一种由28个氨基酸组成的肠道肽,主要在胃底黏膜分泌。1999年,小岛等人将其分离并进行了描述,仅仅三年后,其特异性受体GHSR1a也被鉴定出来。胃饥饿素作为生长激素促分泌素受体的内源性配体,是唯一一种能激活受体的外周促食欲激素,尤其在食欲中枢(下丘脑和垂体)中被发现。胃饥饿素在人体血浆中有两种形式:一种无活性形式称为去酰基胃饥饿素,另一种活性形式称为酰基化胃饥饿素,它是在胃饥饿素O-酰基转移酶(GOAT)的作用下合成的。文献中甚至提到了一个极其复杂的胃饥饿素/GOAT/GHSR系统,该系统参与人体能量调节、新陈代谢以及能量稳态对环境变化的适应。在人类中,血浆胃饥饿素水平在餐前升高,餐后下降,这强烈表明该肽在进食起始过程中发挥生理作用,并且可能用于确定摄入食物的量和质量。除了刺激食物摄入外,胃饥饿素还会导致能量消耗减少,并促进脂肪酸在脂肪细胞中的储存。因此,在人体中,胃饥饿素会引发正能量平衡、肥胖增加以及热量储存增加,这被视为对热量限制条件的一种适应性机制。在当前的世界背景下,当我们目睹食物供应增加且能量消耗降至最低水平时,这些机制已成为致病因素。因此,许多学者和研究人员都接受了胃饥饿素与当前肥胖流行有关的假说。

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