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小鼠中阿片类药物诱导的运动活动的遗传控制。

Genetic control of opiate-induced locomotor activity in mice.

作者信息

Judson B A, Goldstein A

出版信息

J Pharmacol Exp Ther. 1978 Jul;206(1):56-60.

PMID:207859
Abstract

Swiss-Webster stock male and female mice were tested for running activity after a 20 mg/kg dose of levorphanol. The best runners and worst runners were then bred. Within each litter, brother-sister pairs with the highest and lowest running activity after a test dose of levorphanol (20 mg/kg) were segregated and bred. This procedure was followed to the F4 generation. Running activity, analgesia and brain catecholamines were studied. The results showed that the "non-running" (NR) trait segregated at the F1 generation, while the "running" (R) trait diverged more slowly. However, by the third generation, the R mice differed significantly from the F0 stock mice. NR mice also did not show locomotor activity when tested with amphetamine. While the NR mice showed reduced running response to levorphanol they were significantly more sensitive than the F0 stock to the analgesic effect. Measurement of brain catecholamines showed no difference between R and NR mice in dopamine or serotonin, but did show a significant increase in norepinephrine in the NR strain.

摘要

对瑞士韦伯斯特品系的雄性和雌性小鼠注射20毫克/千克剂量的左啡诺后,测试其跑步活动能力。然后挑选出跑得最快和最慢的小鼠进行繁殖。在每一窝中,将注射测试剂量左啡诺(20毫克/千克)后跑步活动能力最高和最低的兄妹配对进行隔离繁殖。这一过程持续到F4代。对跑步活动能力、镇痛作用和脑内儿茶酚胺进行了研究。结果表明,“不跑步”(NR)性状在F1代出现分离,而“跑步”(R)性状的分离则较为缓慢。然而,到第三代时,R小鼠与F0代品系小鼠有显著差异。用苯丙胺测试时,NR小鼠也未表现出运动活性。虽然NR小鼠对左啡诺的跑步反应降低,但它们对镇痛作用的敏感性明显高于F0代品系小鼠。脑内儿茶酚胺的测量结果显示,R小鼠和NR小鼠在多巴胺或5-羟色胺方面没有差异,但NR品系中的去甲肾上腺素显著增加。

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