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纳曲酮可逆性抑制孤立攻击小鼠的疼痛。

Naltrexone-reversible pain suppression in the isolated attacking mouse.

作者信息

Siegfried B, Frischknecht H R

机构信息

Institute of Pharmacology, University of Zurich, Switzerland.

出版信息

Behav Neural Biol. 1988 Nov;50(3):354-60. doi: 10.1016/s0163-1047(88)91082-5.

Abstract

Fighting pairs of isolated DBA/2 mice showed a significant increase in tail-flick response latencies independent of whether opponents were losing or winning the combat. The effect lasted less than 10 min in both animals. Elevated pain thresholds were also found in isolates that attacked a nonaggressive conspecific, and were prevented by naltrexone (0.2 mg/kg), while a larger dose (1.0 mg/kg) inhibited the attack behavior. A small increase in pain threshold was observed after exposure of isolates to the test box alone, while isolation per se had no effect on baseline tail-flick latencies. The data demonstrate that endogenous pain suppressing systems are activated during attack and suggest that this opioid-mediated antinociception is a correlate of the isolation syndrome, reflecting enhanced arousal of the attacking animal.

摘要

单独饲养的DBA/2小鼠打斗时,无论对手在战斗中是输是赢,其甩尾反应潜伏期均显著增加。这种效应在两只动物身上持续时间均不到10分钟。在攻击无攻击性同种动物的单独饲养小鼠中也发现痛阈升高,且可被纳曲酮(0.2毫克/千克)阻断,而较大剂量(1.0毫克/千克)则抑制攻击行为。单独将单独饲养小鼠置于测试箱后,可观察到痛阈略有升高,而单独饲养本身对基线甩尾潜伏期无影响。数据表明,内源性疼痛抑制系统在攻击过程中被激活,提示这种阿片类物质介导的抗伤害感受与隔离综合征相关,反映出攻击动物的觉醒增强。

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