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外侧下丘脑、伏隔核壳和腹侧被盖区中 MC4-R 信号对食物摄入的控制:与乙醇的相互作用。

Control of food intake by MC4-R signaling in the lateral hypothalamus, nucleus accumbens shell and ventral tegmental area: interactions with ethanol.

机构信息

Departamento de Neurociencia y Ciencias de Salud, Universidad de Almería, Almería, 04120, Spain.

出版信息

Behav Brain Res. 2012 Sep 1;234(1):51-60. doi: 10.1016/j.bbr.2012.06.006. Epub 2012 Jun 17.

Abstract

The melanocortin system is involved in animal models of obesity and anorexia-cachexia and MC4 receptors (MC4-R) are currently a target system for the development of drugs aimed to treat obesity and eating disorders in humans. Previous evidence suggest that feeding peptides might lack their orexigenic activity while stimulate ethanol intake. The present study comparatively evaluated food intake (4-h interval) in Sprague-Dawley (SD) rats drinking ethanol (6% w/v, 2 bottle choice paradigm) (EE group) and ethanol-naïve (EN) rats in response to bilateral infusion of the selective MC4-R antagonist HS014 (0, 0.02 or 0.05 μg/0.5 μl/site) or the selective MC4-R agonist cyclo(NH-CH(2)-CH(2)-CO-His-d-Phe-Arg-Trp-Glu)-NH(2) (0, 0.75 or 1.5 μg/0.5 μl/site), into the lateral hypothalamus (LH), the nucleus accumbens (NAc), or the ventral tegmental area (VTA). The main findings in the study are: (1) LH-infusions of the MC4-R antagonist increased and the agonist reduced feeding and total calories consumed, while ethanol intake remained unaltered. (2) NAc- and VTA-infusions of the selective agonist reduced food, ethanol and total calories intake. (3) NAc- and VTA-infusions of the MC4-R antagonist increased feeding in EN rats, but not in EE animals which showed a mild increase in ethanol intake, while total calories consumed remained unaltered. Present data show that having ethanol available reduces feeding elicited by NAc and VTA-MC4-R blockade. Additionally, while MC4-R signaling in the LH appears to modulate homeostatic aspects of feeding, it may contribute to non-homeostatic aspects of ingestive behaviors in the VTA and the NAc.

摘要

黑素皮质素系统参与肥胖症和恶病质厌食症的动物模型,MC4 受体(MC4-R)目前是开发用于治疗人类肥胖症和进食障碍的药物的目标系统。先前的证据表明,摄食肽可能缺乏它们的食欲刺激活性,同时刺激乙醇摄入。本研究比较评估了 Sprague-Dawley(SD)大鼠(SD 大鼠)的食物摄入量(4 小时间隔),这些大鼠饮用乙醇(6%w/v,2 瓶选择范式)(EE 组)和乙醇-naïve(EN)大鼠对选择性 MC4-R 拮抗剂 HS014(0、0.02 或 0.05μg/0.5μl/部位)或选择性 MC4-R 激动剂环(NH-CH2-CH2-CO-His-d-Phe-Arg-Trp-Glu)-NH2(0、0.75 或 1.5μg/0.5μl/部位)双侧侧脑室(LH)、伏隔核(NAc)或腹侧被盖区(VTA)的灌注。研究中的主要发现是:(1)LH 内注射 MC4-R 拮抗剂增加,激动剂减少摄食和总热量消耗,而乙醇摄入保持不变。(2)NAc 和 VTA 内注射选择性激动剂减少食物、乙醇和总热量摄入。(3)NAc 和 VTA 内注射 MC4-R 拮抗剂增加了 EN 大鼠的摄食,但 EE 动物的摄食没有增加,EE 动物的乙醇摄入量略有增加,而总热量消耗保持不变。目前的数据表明,有乙醇可减少 NAc 和 VTA-MC4-R 阻断引起的摄食。此外,虽然 LH 中的 MC4-R 信号似乎调节摄食的稳态方面,但它可能有助于 VTA 和 NAc 中摄食行为的非稳态方面。

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