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首页> 外文期刊>Journal of neuroendocrinology >Chronic Central Administration of Apelin-13 Over 10 Days Increases Food Intake, Body Weight, Locomotor Activity and Body Temperature in C57BL/6 Mice.
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Chronic Central Administration of Apelin-13 Over 10 Days Increases Food Intake, Body Weight, Locomotor Activity and Body Temperature in C57BL/6 Mice.

机译:Apelin-13的慢性中央给药超过10天会增加C57BL / 6小鼠的食物摄入,体重,运动能力和体温。

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The peptide apelin has been located in a wide range of tissues, including the gastrointestinal tract, stomach and adipose tissue. Apelin and its receptor has also been detected in the arcuate and paraventricular nuclei of the hypothalamus, which are involved in the control of feeding behaviour and energy expenditure. This distribution suggests apelin may play a role in energy homeostasis, but previous attempts to discern the effects of apelin by acute injection into the brain have yielded conflicting results. We examined the effect of a chronic 10-day intracerebroventricular (i.c.v.) infusion of apelin-13 into the third ventricle on food intake, body temperature and locomotor activity in C57BL/6 mice. Apelin-13 (1 microg/day) increased food intake significantly on days 3-7 of infusion; thereafter, food intake of treated and control individuals converged. This convergence was potentially because of progressive conversion of apelin-13 to [Pyr(1)]apelin-13 which has a four-fold lower receptor binding affinity at the orphan G protein-coupled receptor, APJ. Locomotor activity was also higher in the apelin-treated mice, especially during the nocturnal peak, when most feeding occurs, and the first hours of the light phase. Body temperature was also elevated during this increased period of activity, but was otherwise unaffected. Apelin-13-infused animals gained more weight than the saline-infused controls, suggesting the elevated locomotor activity did not offset the increased food intake. Elevated locomotion and the consequent increases in body temperature were probably secondary effects to the increased food intake. These results suggest that apelin-13 may play a central role in the control of feeding behaviour and is one of only two peripheral ligands known to stimulate rather than inhibit intake. As apelin production is elevated during obesity, this may provide an important feed-forward mechanism exacerbating the problem. Antagonists of the apelin receptor may therefore be useful pharmaceuticals in the treatment of obesity.
机译:肽apelin已存在于广泛的组织中,包括胃肠道,胃和脂肪组织。在下丘脑的弓形和室旁核中也检测到了Apelin及其受体,它们参与了进食行为和能量消耗的控制。这种分布表明,apelin可能在能量稳态中起作用,但是先前通过急性注入大脑来辨别apelin的作用的尝试产生了矛盾的结果。我们检查了C57BL / 6小鼠向第三脑室长期注入10天的脑室内(i.c.v.)apelin-13对食物摄入,体温和运动能力的影响。输注3-7天时,Apelin-13(每天1微克)可显着增加食物摄入量;此后,治疗和对照个体的食物摄入量趋于一致。这种收敛可能是由于apelin-13逐步转化为[Pyr(1)] apelin-13所致,该蛋白在孤儿G蛋白偶联受体APJ上的受体结合亲和力降低了四倍。在用Apelin处理的小鼠中,自发活动也较高,尤其是在夜间高峰期(大多数进食发生时)和轻度阶段的头几个小时。在此增加的活动期间内,体温也升高了,但不受影响。输注Apelin-13的动物比输注盐水的对照组体重增加,这表明运动能力的提高不能抵消食物摄入量的增加。运动的增加和随后体温的升高可能是食物摄入量增加的次要影响。这些结果表明,apelin-13可能在控制进食行为中发挥重要作用,并且是已知的两个刺激而不是抑制摄取的外围配体之一。由于肥胖期间apelin的产量增加,这可能提供了一个重要的前馈机制,加剧了这一问题。因此,apelin受体的拮抗剂可用于治疗肥胖症。

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