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行为因素在苯二氮䓬类药物咪达唑仑耐受性形成中的作用分析

Analysis of the role of behavioural factors in the development of tolerance to the benzodiazepine midazolam.

作者信息

Griffiths J W, Goudie A J

出版信息

Neuropharmacology. 1987 Feb-Mar;26(2-3):201-9. doi: 10.1016/0028-3908(87)90210-3.

DOI:10.1016/0028-3908(87)90210-3
PMID:3587532
Abstract

Two experiments were conducted on the acute and chronic effects of the short-acting benzodiazepine midazolam on fixed ratio schedule-maintained operant responding in rats. Acute administration of midazolam produced suppression of responding in large doses but elevation of responding in small doses. Following intermittent (every third day) chronic treatment tolerance developed rapidly to the rate-suppressant effects of large doses of midazolam but did not develop to the rate-elevating effects of small doses, even after chronic treatment with large doses of the drug. Thus, when tolerance was measured in terms of shifts in dose-effect curves, it was manifested as a non-parallel shift in the curve after chronic treatment. Since tolerance developed to the effects of large but not small doses, the observed tolerance could not be attributed to changes in disposition of the drug. The development of tolerance did not depend on whether the drug was given before or after behavioural testing. These findings contrast with data reported in behavioural studies with other sedative-hypnotics (ethanol, barbiturates). Animals tolerant to midazolam showed no cross-tolerance to ethanol, a drug for which there is reliable evidence indicating that behavioural factors play a role in acquisition of tolerance. Tolerance to midazolam cannot therefore be explained in terms of learned strategies acquired as a result of drug-induced loss of rewarding stimuli. This conclusion contrasts with recent suggestions (File, 1985; File and Pellow, 1985) that tolerance to benzodiazepines may be mediated by instrumental conditioning processes.

摘要

进行了两项实验,研究短效苯二氮䓬类药物咪达唑仑对大鼠固定比率强化程式维持的操作性反应的急性和慢性影响。急性给予咪达唑仑时,大剂量会抑制反应,但小剂量会增强反应。间歇性(每三天一次)慢性给药后,对大剂量咪达唑仑的反应抑制作用迅速产生耐受性,但对小剂量的反应增强作用即使在大剂量药物慢性治疗后也未产生耐受性。因此,当根据剂量-效应曲线的变化来测量耐受性时,慢性治疗后曲线表现为非平行移动。由于对大剂量而非小剂量的效应产生了耐受性,观察到的耐受性不能归因于药物处置的变化。耐受性的产生并不取决于药物是在行为测试之前还是之后给予。这些发现与其他镇静催眠药(乙醇、巴比妥类药物)行为学研究报告的数据形成对比。对咪达唑仑产生耐受性的动物对乙醇没有交叉耐受性,有可靠证据表明乙醇的行为因素在耐受性的获得中起作用。因此,咪达唑仑的耐受性不能用药物诱导的奖励刺激丧失所获得的学习策略来解释。这一结论与最近的观点(法尔,1985年;法尔和佩洛,1985年)形成对比,即对苯二氮䓬类药物的耐受性可能由工具性条件作用过程介导。

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