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纳洛酮对大鼠饮水行为的抑制作用:进一步的特征研究。

Suppression of drinking by naloxone in the rat: a further characterization.

作者信息

Brown D R, Holtzman S G

出版信息

Eur J Pharmacol. 1981 Jan 29;69(3):331-40. doi: 10.1016/0014-2999(81)90479-9.

Abstract

The effects of naloxone, an opiate antagonist, were examined on drinking induced by various dipsogenic stimuli. In rats deprived of water for 24 h, naloxone (0.1-10 mg/kg) produced a dose-related suppression of drinking immediately following water presentation but did not alter the latency to begin drinking. Naloxone also produced a dose-related suppression of water consumption induced by isoproterenol and angiotensin II, agents simulating conditions of extracellular dehydration. Naltrexone, a congener of naloxone, was more potent than naloxone in reducing isoproterenol-induced water intake. Schedule-induced polydipsia, which occurs in the absence of body fluid deficits, was not altered by either naloxone or naltrexone at doses attenuating drinking induced by the other methods. These data suggest that the suppressant effects of naloxone on water consumption are not a manifestation of an increased latency to drink or an impairment in the motor components of drinking activity. Furthermore, narcotic antagonists appear to attenuate regulatory, but not adjunctive drinking.

摘要

研究了阿片拮抗剂纳洛酮对各种致渴刺激所诱导饮水的影响。在禁水24小时的大鼠中,纳洛酮(0.1 - 10毫克/千克)在给予水后立即产生剂量相关的饮水抑制,但并未改变开始饮水的潜伏期。纳洛酮还对异丙肾上腺素和血管紧张素II诱导的饮水产生剂量相关的抑制作用,这两种物质模拟细胞外脱水状态。纳洛酮的同类物纳曲酮在减少异丙肾上腺素诱导的饮水量方面比纳洛酮更有效。在不存在体液缺乏情况下发生的程序性诱导多饮,在给予能减弱其他方法诱导饮水的剂量时,纳洛酮或纳曲酮均未对其产生影响。这些数据表明,纳洛酮对饮水的抑制作用并非饮水潜伏期延长或饮水活动运动成分受损的表现。此外,阿片拮抗剂似乎减弱了调节性饮水,但未减弱辅助性饮水。

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