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比较C75经中枢和外周给药对食物摄入量、体重及条件性味觉厌恶的影响。

Comparison of central and peripheral administration of C75 on food intake, body weight, and conditioned taste aversion.

作者信息

Clegg Deborah J, Wortman Matt D, Benoit Stephen C, McOsker Charles C, Seeley Randy J

机构信息

Department of Psychiatry, University of Cincinnati, Cincinnati, Ohio, USA.

出版信息

Diabetes. 2002 Nov;51(11):3196-201. doi: 10.2337/diabetes.51.11.3196.

Abstract

Mice respond to fatty acid synthase (FAS) inhibitors by profoundly reducing their food intake and body weight. Evidence indicates that the central nervous system (CNS) may be the critical site of action; however, a peripheral contribution cannot be ruled out. We compared doses of the FAS inhibitor C75 in the CNS (third ventricle [i3vt]) and periphery (intraperitoneal [IP]) to reduce food intake and body weight in rats. Centrally, the threshold dose was 3 micro g, whereas a dose of 10 mg/kg was required peripherally. Such data argue for FAS activity in the CNS as a potent target for the actions of C75. To control for nonspecific effects of FAS inhibition, we compared C75 administration in two models of illness, conditioned taste aversion and need-induced sodium appetite. Our results suggest the anorexia produced by IP C75 is accompanied by visceral illness, whereas the anorexia produced by i3vt is not. In addition, we placed animals in an indirect calorimeter after an IP injection of C75. We found that consistent with behavioral measures of visceral illness, peripheral C75 reduced heat expenditure and resulted in animals losing less weight than fasted control animals, suggesting that peripherally administered C75 has aversive properties. Understanding the mechanisms by which FAS inhibition in the CNS reduces food intake could lead to specific targets for the manipulation of energy balance and the treatment of obesity.

摘要

小鼠对脂肪酸合酶(FAS)抑制剂的反应是大幅减少食物摄入量和体重。有证据表明,中枢神经系统(CNS)可能是关键作用部位;然而,外周的作用也不能排除。我们比较了FAS抑制剂C75在中枢神经系统(第三脑室[i3vt])和外周(腹腔内[IP])给药时降低大鼠食物摄入量和体重的剂量。在中枢,阈值剂量为3微克,而在外周则需要10毫克/千克的剂量。这些数据表明中枢神经系统中的FAS活性是C75发挥作用的有效靶点。为了控制FAS抑制的非特异性作用,我们在两种疾病模型(条件性味觉厌恶和需求诱导的钠食欲)中比较了C75的给药情况。我们的结果表明,腹腔注射C75产生的厌食症伴有内脏疾病,而第三脑室注射产生的厌食症则不然。此外,我们在腹腔注射C75后将动物置于间接热量计中。我们发现,与内脏疾病的行为测量结果一致,外周注射C75会降低热量消耗,导致动物体重减轻比禁食对照动物少,这表明外周给药的C75具有厌恶特性。了解中枢神经系统中FAS抑制减少食物摄入的机制可能会为调节能量平衡和治疗肥胖症找到特定靶点。

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