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首页> 外文期刊>American Journal of Physiology >GLP-1 receptor signaling contributes to anorexigenic effect of centrally administered oxytocin in rats.
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GLP-1 receptor signaling contributes to anorexigenic effect of centrally administered oxytocin in rats.

机译:GLP-1受体信号传导有助于在大鼠中集中施用催产素的镇痛作用。

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摘要

The present study examined possible interactions between central glucagon-like peptide-1 (GLP-1) and oxytocin (OT) neural systems by determining whether blockade of GLP-1 receptors attenuates OT-induced anorexia and vice versa. Male rats were acclimated to daily 4-h food access. In the first experiment, rats were infused centrally with GLP-1 receptor antagonist or vehicle, followed by an anorexigenic dose of synthetic OT. Access to food began 20 min later. Cumulative food intake was measured every 30 min for 4 h. In the second experiment, rats were infused with OT receptor blocker or vehicle, followed by synthetic GLP-1 [(7-36) amide]. Subsequent food intake was monitored as before. The anorexigenic effect of OT was eliminated in rats pretreated with the GLP-1 receptor antagonist. Conversely, GLP-1-induced anorexia was not affected by blockade of OT receptors. In a separate immunocytochemical study, OT-positive terminals were found closely apposed to GLP-1-positive perikarya, and central infusion of OTactivated c-Fos expression in GLP-1 neurons. These findings implicate endogenous GLP-1 receptor signaling as an important downstream mediator of anorexia in rats after activation of central OT neural pathways.
机译:本研究通过确定对GLP-1受体的阻滞是否减弱了OT引起的厌食症,从而研究了中央胰高血糖素样肽1(GLP-1)和催产素(OT)神经系统之间的可能相互作用。使雄性大鼠适应每天4小时的食物摄取。在第一个实验中,将GLP-1受体拮抗剂或媒介物集中输注给大鼠,然后再注入一定剂量的合成OT来产生镇痛作用。 20分钟后开始获取食物。每30分钟测量一次4小时的累积食物摄入量。在第二个实验中,向大鼠灌输OT受体阻滞剂或赋形剂,然后合成GLP-1 [(7-36)酰胺]。像以前一样监测随后的食物摄入量。在用GLP-1受体拮抗剂预处理的大鼠中,OT的厌食作用被消除。相反,GLP-1诱导的厌食症不受OT受体阻滞的影响。在另一项免疫细胞化学研究中,发现OT阳性末端与GLP-1阳性周核细胞紧密相关,并在GLP-1神经元中集中注入OT激活的c-Fos表达。这些发现暗示内源性GLP-1受体信号传导是中枢OT神经通路激活后大鼠厌食症的重要下游介质。

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