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乙醛对嗜酒大鼠腹侧被盖区后部的强化作用。

The reinforcing effects of acetaldehyde in the posterior ventral tegmental area of alcohol-preferring rats.

作者信息

Rodd-Henricks Zachary A, Melendez Roberto I, Zaffaroni Alejandro, Goldstein Avram, McBride William J, Li Ting-Kai

机构信息

Department of Psychiatry, Institute of Psychiatric Research, Indiana University School of Medicine, 791 Union Drive, Indianapolis, IN 46202-4887, USA.

出版信息

Pharmacol Biochem Behav. 2002 May;72(1-2):55-64. doi: 10.1016/s0091-3057(01)00733-x.

Abstract

Acetaldehyde (ACD), the first metabolite of ethanol, is a biologically active compound, which may mediate some of the reinforcing, behavioral and neurotoxic effects of ethanol. The objective of this study was to test the hypothesis that ACD is reinforcing within the mesolimbic system. The intracranial self-administration (ICSA) technique was employed to determine whether ACD was reinforcing in the posterior ventral tegmental area (VTA), a site that supports the reinforcing actions of ethanol. Adult female alcohol-preferring (P) rats were implanted with guide cannulae aimed at the posterior VTA. Subjects were placed in two-lever operant chambers 7-10 days after surgery. Responding on the "active lever" on a fixed ratio 1 (FR1) schedule of reinforcement caused the delivery of 100 nl of infusate, whereas responses on the "inactive lever" were without consequences. Rats were assigned to one of five groups that self-administered either artificial cerebrospinal fluid (aCSF) throughout all eight sessions (4 h in duration) or 3- and 6-, 11- and 23-, 45- and 90- or 180- and 360-microM ACD for the eight sessions, with the lower concentration of ACD given for the initial four sessions and the higher concentration of ACD given for the last four sessions. A second experiment examined the acquisition (first four sessions), extinction (aCSF in sessions 5 and 6) and reinstatement using 90-microM ACD. A third experiment examined the effects of extending the time-out period (from 5 to 55 s) on the number and pattern of infusions of 23-microM ACD. Adult P rats readily self-administered 6-90-microM ACD and discriminated between the active and inactive levers. Furthermore, rats self-administering 90-microM ACD also demonstrated extinction behavior when aCSF was substituted for ACD and gradually reinstated active lever responding when ACD was reintroduced. P rats maintained similar numbers of infusions and infusion patterns under both time-out schedules. Overall, the data indicate that ACD is a potent reinforcer within the posterior VTA of the P rat.

摘要

乙醛(ACD)是乙醇的首个代谢产物,是一种生物活性化合物,它可能介导乙醇的一些强化、行为及神经毒性作用。本研究的目的是检验乙醛在中脑边缘系统内具有强化作用这一假设。采用颅内自我给药(ICSA)技术来确定乙醛在腹侧被盖区后部(VTA)是否具有强化作用,该部位支持乙醇的强化作用。成年雌性嗜酒(P)大鼠植入了指向VTA后部的引导套管。术后7 - 10天,将实验对象置于双杠杆操作箱中。按照固定比率1(FR1)强化程序对“主动杠杆”做出反应会导致注入100微升灌流液,而对“非主动杠杆”做出反应则没有任何结果。大鼠被分为五组,其中一组在全部八节实验(持续4小时)中均自我给药人工脑脊液(aCSF),另外四组分别在八节实验中自我给药3微摩尔和6微摩尔、11微摩尔和23微摩尔、45微摩尔和90微摩尔或180微摩尔和360微摩尔的乙醛,初始四节实验给予较低浓度的乙醛,最后四节实验给予较高浓度的乙醛。第二个实验考察了获取阶段(前四节实验)、消退阶段(第五节和第六节实验给予aCSF)以及使用90微摩尔乙醛进行恢复阶段的情况。第三个实验考察了将超时时间从5秒延长至55秒对23微摩尔乙醛注入次数和模式的影响。成年P大鼠很容易自我给药6 - 90微摩尔的乙醛,并能区分主动杠杆和非主动杠杆。此外,自我给药90微摩尔乙醛的大鼠在aCSF替代乙醛时也表现出消退行为,当重新引入乙醛时,又逐渐恢复对主动杠杆的反应。在两种超时时间表下,P大鼠保持了相似的注入次数和注入模式。总体而言,数据表明乙醛在P大鼠的VTA后部是一种有效的强化剂。

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