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Effects of orexins on energy balance and thermoregulation.

机译:食欲素对能量平衡和温度调节的影响。

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Intracerebroventricular injections of 10-20-microg orexin-A induce food intake in rats for about 30 min, or enhance fasting-induced hyperphagia. In thermoregulatory studies, an amount of 2 microg of the peptide causes hypometabolism and hypothermia in the same period. The thermoregulatory reaction can be demonstrated at moderately cool environments, mainly after slight food deprivation. Both the ingestive and the thermoregulatory reactions are more pronounced in cold-adapted animals. Pretreatment with D-Tyr27,36,D-Thr32-NPY(27-36), a peptide-antagonist of NPY, prevents the hypothermia. It is concluded that, probably through NPY activation, orexin-A is involved primarily in the regulation of energy status of the body (as an anabolic agent), and not simply in the regulation of either food intake or body temperature. This anabolic response is followed by a late and more sustained catabolic phase characterized by absence of food intake, increased metabolism and dose-dependent hyperthermia, which hyperthermia cannot be suppressed by the NPY-antagonist. In contrast to orexin-A, neither hyperphagia nor suppression of refeeding hyperphagia, but dose-dependent hyperthermia follows injections of orexin-B, suggesting that this peptide has neither coordinated anabolic nor coordinated catabolic effects on energy balance.
机译:脑室内注射10-20微克orexin-A可使大鼠进食约30分钟,或增强空腹诱发的食欲亢进。在温度调节研究中,在同一时期内,2微克的肽量会引起代谢不足和体温过低。可以在中等凉爽的环境中证明温度调节反应,主要是在食物被轻度剥夺之后。摄食反应和体温调节反应在适应寒冷的动物中更为明显。用D-Tyr27,36,D-Thr32-NPY(27-36)(NPY的肽拮抗剂)进行预处理可防止体温过低。结论是,可能通过NPY激活,orexin-A主要参与了人体能量状态的调节(作为合成代谢药物),而不仅仅是参与食物摄入或体温的调节。在该合成代谢反应之后,是分解代谢后期且持续时间更长,其特征是缺乏食物摄入,新陈代谢增加和剂量依赖性热疗,而NPY拮抗剂不能抑制该热疗。与食欲素A相比,食欲素B注射后既没有食欲亢进也没有抑制进食性食欲亢进,但是剂量依赖性体温过高,表明该肽对能量平衡既没有协同代谢也没有分解代谢作用。

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