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Acute morphine dependence in mice selectively-bred for high and low analgesia.

机译:选择性吗啡对小鼠的急性吗啡依赖性进行高和低镇痛。

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摘要

Acute morphine dependence was compared in mice selectively-bred for high (HA) and low (LA) swim stress-induced analgesia and high (HAR) and low (LAR) levorphanol analgesia by counting the number of naloxone-precipitated jumps. Whereas LAR mice displayed greater acute morphine dependence than HAR mice, HA and LA mice did not differ. No genotypic differences were observed in non-dependent mice, discounting possible differences in basal naloxone sensitivity and/or opioid peptide levels. Thus, the two selection projects, while both producing lines exhibiting highly divergent sensitivity to morphine analgesia, have not had analogous effects on all opioid measures, supporting the notion of independent genetic mediation of opioid analgesia and dependence. Further, these data suggest that analgesic sensitivity may not predict sensitivity to morphine dependence.
机译:通过计算纳洛酮沉淀的跳跃次数,比较了选择性吗啡对高(HA)和低(LA)游泳应激诱导的镇痛以及高(HAR)和低(LAR)左啡烷镇痛的小鼠的急性吗啡依赖性。 LAR小鼠比HAR小鼠表现出更高的急性吗啡依赖性,而HA和LA小鼠没有差异。在非依赖性小鼠中未观察到基因型差异,消除了基础纳洛酮敏感性和/或阿片样物质肽水平的可能差异。因此,两个选择项目虽然都对吗啡镇痛表现出高度不同的敏感性,但并未对所有阿片类药物措施产生类似影响,从而支持了阿片类药物镇痛和依赖性的独立遗传介导概念。此外,这些数据表明,止痛药的敏感性可能无法预测对吗啡依赖的敏感性。

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