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尿皮质素、促肾上腺皮质激素释放因子-2受体与能量平衡。

Urocortin, corticotropin releasing factor-2 receptors and energy balance.

作者信息

Cullen M J, Ling N, Foster A C, Pelleymounter M A

机构信息

Department of Neuroscience, Neurocrine Biosciences, Inc., San Diego, California 92121, USA.

出版信息

Endocrinology. 2001 Mar;142(3):992-9. doi: 10.1210/endo.142.3.7989.

Abstract

Although there is considerable information regarding the role of brain CRF in energy balance, relatively little is known about the role of urocortin (UCN), which is an equally potent anorexic agent. Therefore, the effects of intracerebroventricular (icv) administration of UCN (0.01-1 nmol/day) on food intake and body weight were assessed over a period of 13 days and compared with data from CRF-infused counterparts. Although both peptides dose dependently reduced food intake and weight gain, the effects of CRF were much greater in magnitude than those of UCN, particularly on body weight. Pair-feeding studies suggested that, while the effects of CRF on body weight could not be completely explained by appetite suppression, the effects of UCN appeared to be due to its initial impact on food intake. CRF increased brown adipose fat pad and adrenal weights, whereas it reduced thymus and spleen weights. CRF also increased serum corticosterone, triglyceride, FFA, and cholesterol levels, whereas it reduced glucose. UCN did not produce any consistent changes in any of these indices of sympathetic nervous system activation. Concurrent administration of the CRF(2)-selective antagonist, antisauvagine-30 (ASV-30) (30 nmol/day) completely reversed or attenuated the effects of UCN and CRF (1 nmol/day) on food intake and body weight. ASV-30 did not significantly attenuate any of the above CRF-induced changes in tissue weights or serum chemistry. These data suggest that the central CRF(2) receptor may primarily mediate the anorexic, but not the metabolic effects of CRF.

摘要

尽管关于脑促肾上腺皮质激素释放因子(CRF)在能量平衡中的作用已有大量信息,但对于同样强效的厌食剂尿皮质素(UCN)的作用却知之甚少。因此,在13天的时间里评估了脑室内(icv)注射UCN(0.01 - 1 nmol/天)对食物摄入量和体重的影响,并与注射CRF的对照组数据进行了比较。尽管两种肽都呈剂量依赖性地减少食物摄入量和体重增加,但CRF的作用在程度上比UCN大得多,尤其是对体重的影响。配对喂养研究表明,虽然CRF对体重的影响不能完全通过食欲抑制来解释,但UCN的作用似乎是由于其对食物摄入量的初始影响。CRF增加了棕色脂肪垫和肾上腺重量,而降低了胸腺和脾脏重量。CRF还增加了血清皮质酮、甘油三酯、游离脂肪酸(FFA)和胆固醇水平,而降低了葡萄糖水平。UCN在交感神经系统激活的任何这些指标上均未产生任何一致的变化。同时给予CRF(2)选择性拮抗剂抗蛙皮素-30(ASV-30)(30 nmol/天)可完全逆转或减弱UCN和CRF(1 nmol/天)对食物摄入量和体重的影响。ASV-30并未显著减弱上述任何CRF诱导的组织重量或血清化学变化。这些数据表明,中枢CRF(2)受体可能主要介导CRF的厌食作用,而非代谢作用。

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