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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Naloxone-precipitated withdrawal jumping in 11 inbred mouse strains: evidence for common genetic mechanisms in acute and chronic morphine physical dependence.
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Naloxone-precipitated withdrawal jumping in 11 inbred mouse strains: evidence for common genetic mechanisms in acute and chronic morphine physical dependence.

机译:纳洛酮在11种近交小鼠品系中引起的戒断跳动:急性和慢性吗啡物理依赖性的常见遗传机制的证据。

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摘要

Physical dependence is a widely known consequence of morphine intake. Although commonly associated with prolonged or repeated morphine administration, withdrawal symptoms can be elicited even after a single prior morphine exposure. What remains contentious is the extent to which physical dependence following acute and chronic morphine treatment is mediated by common physiological substrates and, accordingly, represent distinct syndromes. The genetic relationship between acute and chronic morphine dependence was thus presently studied by comparing mice of 11 inbred strains (129P3, A, AKR, BALB/c, C3H/He, C57BL/6, CBA, DBA/2, LP, SJL, and SWR) for naloxone-precipitated withdrawal jumping responses using three subcutaneous morphine administration paradigms: acute (single injection) or chronic (three daily morphine injections for 4 days) injection, or chronic infusion (7 days via implanted osmotic minipumps). Although there were differences in the magnitude of withdrawal jumping between the three different morphine administration paradigms, large and significant strain differences were observed for each. In addition, the same strains were unusually sensitive or, conversely, altogether refractory to withdrawal jumping across all morphine treatment conditions. Overall, strain jumping means between acute and chronic dependence paradigms displayed a high degree of genetic correlation (r=0.87-0.95). The significant correlation between chronic morphine injection and continuous morphine infusion discounts the possible confounding effect of contextual learning and spontaneous withdrawal between chronic injections on the assessment of naloxone-precipitated withdrawal. Substantial heritability was also observed for acute and both paradigms of chronic dependence, with estimates ranging from h(2)=0.53 to 0.70.The present demonstration of a strong genetic correlation between physical dependence to morphine following acute and chronic treatment implies that genes associated with variable sensitivity in the two traits are the same, and is suggestive of shared physiological substrates. The data also demonstrate that the differential genetic liability to morphine physical dependence begins with, and is predicted by, the first morphine exposure.
机译:身体依赖性是吗啡摄入的众所周知的结果。尽管通常与吗啡的长期或反复给药有关,但即使在事先接受一次吗啡暴露后,也会引起戒断症状。仍然存在争议的是,急性和慢性吗啡治疗后的身体依赖性在多大程度上由共同的生理底物介导,并因此代表了不同的综合症。因此,目前通过比较11种自交系(129P3,A,AKR,BALB / c,C3H / He,C57BL / 6,CBA,DBA / 2,LP,SJL和SWR)可使用三种皮下注射吗啡给药方式处理纳洛酮引起的戒断跳跃反应:急性(单次注射)或慢性(每天3次吗啡注射4天)注射或慢性输注(通过植入的渗透性微型泵7天)。尽管在三种不同的吗啡给药范例之间,戒断跳跃的幅度存在差异,但每种观察到的应变差异都很大。此外,相同的菌株对所有吗啡治疗条件下的跳跃跳跃都异常敏感或相反。总体而言,急性和慢性依赖范例之间的应变跳跃方式显示出高度的遗传相关性(r = 0.87-0.95)。慢性吗啡注射液和连续吗啡注射液之间的显着相关性使长期注射之间的情境学习和自发戒断对纳洛酮沉淀戒断的评估可能产生混淆作用。在急性和慢性依赖的两个范例中也观察到了显着的遗传力,估计范围从h(2)= 0.53至0.70。本研究表明,急性和慢性治疗后物理依赖与吗啡之间存在很强的遗传相关性,表明与这两个性状的可变敏感性是相同的,并且暗示了共有的生理底物。数据还表明,对吗啡物理依赖性的差异遗传易感性始于第一次吗啡暴露,并通过首次暴露来预测。

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