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胰高血糖素样肽-1(7-36)酰胺:饱腹感和内感受性应激的中枢调节因子。

Glucagon-like peptide-1 (7-36) amide: a central regulator of satiety and interoceptive stress.

作者信息

van Dijk G, Thiele T E

机构信息

Department of Animal Physiology, University of Groningen, The Netherlands.

出版信息

Neuropeptides. 1999 Oct;33(5):406-14. doi: 10.1054/npep.1999.0053.

Abstract

Glucagon-like peptide-1 (7-36) amide (GLP-1) is processed from proglucagon in the distal ileum as well as in the CNS. In the periphery, GLP-1 acts as an incretin factor and profoundly inhibits upper gastrointestinal motility ('ileal brake'), the latter presumably involving the CNS. Within the CNS, GLP-1 has a satiating effect, since administration of GLP-1 into the third cerebral ventricle reduces short-term food intake (and meal size), while administration of GLP-1 antagonists have the opposite effect. In addition, activation of GLP-1 receptors in certain brain regions elicits strong taste aversions. Similarities between toxin- and GLP-1-induced neuronal activity in the CNS (brain stem) suggest a role for central GLP-1 receptors in relaying interoceptive stress. Thus, regionally distinct GLP-1 receptor populations in the CNS may be involved in satiety or malaise. It is argued that the satiating and aversive aspects of GLP-1 serve homeostatic and nonhomeostatic functions with respect to maintenance of nutrient balance.

摘要

胰高血糖素样肽-1(7-36)酰胺(GLP-1)在回肠末端以及中枢神经系统中由胰高血糖素原加工而成。在外周,GLP-1作为一种肠促胰岛素因子,可显著抑制上消化道运动(“回肠制动”),后者可能涉及中枢神经系统。在中枢神经系统内,GLP-1具有饱腹感作用,因为向第三脑室注射GLP-1可减少短期食物摄入量(和进餐量),而注射GLP-1拮抗剂则产生相反的效果。此外,在某些脑区激活GLP-1受体会引发强烈的味觉厌恶。毒素诱导和GLP-1诱导的中枢神经系统(脑干)神经元活动之间的相似性表明,中枢GLP-1受体在传递内感受性应激方面发挥作用。因此,中枢神经系统中区域不同的GLP-1受体群体可能参与饱腹感或不适的调节。有人认为,GLP-1的饱腹感和厌恶方面在维持营养平衡方面发挥着稳态和非稳态功能。

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