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联合性和非联合性过程对吗啡耐受性发展的作用。

Contribution of associative and nonassociative processes to the development of morphine tolerance.

作者信息

Tiffany S T, Drobes D J, Cepeda-Benito A

机构信息

Department of Psychological Sciences, Purdue University, West Lafayette, IN 47907.

出版信息

Psychopharmacology (Berl). 1992;109(1-2):185-90. doi: 10.1007/BF02245498.

Abstract

The contribution of associative and nonassociative processes to the development of tolerance to the analgesic effects of morphine in rats was investigated in two experiments. Associative contingencies were manipulated by administering a series of moderately high morphine doses (20 mg/kg) either explicitly paired or explicitly unpaired with a distinctive context. During distinctive context exposures, animals were placed for 60 min in plastic boxes located in a room adjacent to the colony room. The distinctiveness of this environment was enhanced by the presence of white noise and a pine scent. Nonassociative processes were manipulated by administering the morphine at either a very short (6 h) or relatively long (96 h) interdose-interval (IDI). Analgesia was measured on a tail-flick test. At the 96 h IDI, tolerance, as indexed by shifts in dose-response curves, was controlled primarily by associative processes. Associative control over tolerance at the long IDI was evident at an immediate test (experiment 1) and was retained for a 30 day interval (experiment 2). In contrast, tolerance that developed at the 6 h IDI was not influenced by associative contingencies at the immediate test (experiment 1) and showed no retention over a 30 day interval (experiment 2). These data suggest that tolerance that developed at the short IDI was nonassociative. Overall, the results indicate that conditions conductive to the development of non-associative tolerance disrupt the acquisition of associative tolerance. Hypotheses regarding the absence of associative effects at the short IDI are reviewed. Methodological implications of these results for evaluations of associative and nonassociative morphine tolerance are also discussed.

摘要

在两项实验中,研究了联想性和非联想性过程对大鼠吗啡镇痛作用耐受性发展的贡献。通过给予一系列中等高剂量的吗啡(20毫克/千克)来操纵联想性意外情况,这些剂量要么明确地与一个独特的环境配对,要么明确地不与该环境配对。在接触独特环境期间,将动物放置在位于与饲养室相邻房间的塑料盒中60分钟。白噪音和松木香味增强了这种环境的独特性。通过以非常短(6小时)或相对长(96小时)的给药间隔(IDI)给予吗啡来操纵非联想性过程。通过甩尾试验测量镇痛效果。在96小时的给药间隔下,以剂量反应曲线的变化为指标的耐受性主要由联想性过程控制。在即时测试(实验1)中,长给药间隔下对耐受性的联想性控制很明显,并且在30天的间隔内保持(实验2)。相比之下,在6小时给药间隔下产生的耐受性在即时测试(实验1)中不受联想性意外情况的影响,并且在30天的间隔内没有保持(实验2)。这些数据表明,在短给药间隔下产生的耐受性是非联想性的。总体而言,结果表明有利于非联想性耐受性发展的条件会干扰联想性耐受性的获得。回顾了关于短给药间隔下缺乏联想性效应的假设。还讨论了这些结果对联想性和非联想性吗啡耐受性评估的方法学意义。

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