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Varenicline, the clinically effective smoking cessation agent, restores probabilistic response reversal performance during withdrawal from nicotine

机译:Varenicline,临床有效的吸烟戒烟剂,恢复尼古丁戒断期间的概率反应逆转性能

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There is recognition that cognitive problems can contribute to renewed drug taking in former addicts. Our previous work has indicated that current smokers show reduced performance on a probabilistic reversal learning (PRL) task, relative to former smokers. To further explore PRL performance and its relevance to smoking, in addition to the role of nicotine, we developed a model of nicotine withdrawal-induced deficits in rodents. A second goal was to test varenicline, an alpha 4 beta 2 partial agonist, for its ability to restore any cognitive impairment. Acute effects of nicotine and varenicline on PRL performance in non-dependent animals were minimal and confined to speed of responding. When rats were made dependent on nicotine via osmotic minipumps implanted for 7 days (3.16 mg/kg/day), repeated tests at specified withdrawal time points revealed PRL disruption peaking at 12 and 24 hours following surgical removal of minipumps. Withdrawal was characterized by significant deficits in the number of reversals (P < 0.05), speed of responding (P < 0.01) and increases in omissions (P < 0.05). Nicotine (0.2 mg/kg SC) or varenicline (0.3 and 1.0 mg/kg SC) administered 10-minute prior to PRL test sessions during withdrawal, relieved the performance deficits. At 24-hour withdrawal, nicotine and varenicline (1 mg/kg) prevented decrements in reversals, in addition to ameliorating slower speed of responding. The high dose of varenicline only reduced omissions. These results confirm the role of nicotine in withdrawal-induced disruption of PRL performance and suggest that the model may be useful for investigating efficacy of potential new treatments for smoking cessation.
机译:有认识到认知问题可以有助于在前瘾君子的重新吸毒。我们以前的工作表明,目前的吸烟者在相对于前吸烟者的概率逆转学习(PRL)任务上表现出降低的性能。为了进一步探讨PRL的性能及其与吸烟的相关性,除了尼古丁的作用外,我们还开发了啮齿动物中尼古丁戒断诱导的缺陷模型。第二个目标是测试valenicline,α4beta 2部分激动剂,以获得恢复任何认知障碍的能力。尼古丁和狭窄对非依赖性动物中PRL性能的急性作用最小,局限于响应的速度。当通过植入7天的渗透微型泵取决于尼古丁的大鼠(3.16mg / kg /天),在特定的戒断时间点的重复测试显示,在手术移除Minipumps后12和24小时显示PRL破坏。撤回的特征在于逆转数量的显着缺陷(P <0.05),响应速度(P <0.01)并增加遗漏(P <0.05)。尼古丁(0.2mg / kg sc)或varenicline(0.3和1.0mg / kg sc)在撤回期间PRL测试课程前10分钟施用,减轻了性能缺陷。在24小时退出时,除了改善响应速度速度速度较慢的响应速度之外,尼古丁和损伤(1 mg / kg)防止逆转递减。高剂量的varenicline只减少了遗漏。这些结果证实了尼古丁在戒断引起的PRL性能中断中的作用,并表明该模型可用于研究潜在的新治疗戒烟的疗效。

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