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G蛋白偶联受体101 mRNA在小鼠脑中的表达:能量挑战对下丘脑后部和杏仁核中表达的影响

G protein-coupled receptor 101 mRNA expression in the mouse brain: altered expression in the posterior hypothalamus and amygdala by energetic challenges.

作者信息

Nilaweera K N, Ozanne D, Wilson D, Mercer J G, Morgan P J, Barrett P

机构信息

Rowett Research Institute, Aberdeen Centre for Energy Regulation and Obesity (ACERO), Bucksburn, Aberdeen, UK.

出版信息

J Neuroendocrinol. 2007 Jan;19(1):34-45. doi: 10.1111/j.1365-2826.2006.01502.x.

Abstract

GPCR101 is a recently identified orphan G protein-coupled receptor (GPCR) expressed abundantly in the human and mouse hypothalamus. In the absence of a ligand, a direct approach to determine the function(s) of this receptor is not possible. However, clues to the possible functions of GPCR101 may yield from information on the distribution of the receptor and the effect of in vivo manipulation upon the expression level of the receptor. In situ hybridisation on mouse brain sections revealed GPCR101 expression in a number of nuclei, including the amygdala, lateral parabrachial nucleus and nucleus of the solitary tract, as well as in the arcuate nucleus, posterior hypothalamus and paraventricular nucleus of the hypothalamus. Food-deprivation was found to increase GPCR101 mRNA level in the posterior hypothalamus and amygdala. In obese mice bearing the ob gene mutation, GPCR101 mRNA level decreased in the posterior hypothalamus and remained unaltered in the amygdala. By contrast, in both nuclei, GPCR101 mRNA level did not change significantly in obese ob/ob mice after intraperitoneal injection of leptin or in mice fed with a high fat diet. These data suggest that GPCR101 mRNA expression in the posterior hypothalamus and amygdala is regulated by a factor(s) other than leptin. Dual in situ hybridisation was used to establish the relationship between GPCR101 and neuropeptides expressed in the hypothalamus. In the arcuate nucleus, GPCR101 mRNA was expressed in approximately half of the population of neurones expressing the mRNA for the anorexigenic neuropeptide, pro-opiomelanocortin, which suggests a potential functional relationship.

摘要

GPCR101是一种最近发现的孤儿G蛋白偶联受体(GPCR),在人和小鼠的下丘脑大量表达。在没有配体的情况下,直接确定该受体功能的方法是不可能的。然而,关于GPCR101可能功能的线索可能来自于受体分布的信息以及体内操作对受体表达水平的影响。对小鼠脑切片进行原位杂交显示,GPCR101在多个核中表达,包括杏仁核、外侧臂旁核和孤束核,以及下丘脑的弓状核、下丘脑后部和室旁核。发现食物剥夺会增加下丘脑后部和杏仁核中GPCR101 mRNA的水平。在携带ob基因突变的肥胖小鼠中,下丘脑后部GPCR101 mRNA水平下降,而杏仁核中则保持不变。相比之下,在这两个核中,腹腔注射瘦素后肥胖的ob/ob小鼠或喂食高脂肪饮食的小鼠中,GPCR101 mRNA水平没有显著变化。这些数据表明,下丘脑后部和杏仁核中GPCR101 mRNA的表达受瘦素以外的其他因素调节。采用双重原位杂交来建立GPCR101与下丘脑表达的神经肽之间的关系。在弓状核中,GPCR101 mRNA在表达厌食神经肽阿黑皮素原mRNA的约一半神经元群体中表达,这表明存在潜在的功能关系。

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