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Role of α5 Nicotinic Acetylcholine Receptors in Pharmacological and Behavioral Effects of Nicotine in Mice

机译:α5烟碱乙酰胆碱受体在小鼠尼古丁药理和行为作用中的作用

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摘要

Incorporation of the α5 nicotinic acetylcholine receptor (nAChR) subunit can greatly influence nAChR function without altering receptor number. Although few animal studies have assessed the role of the α5 nAChR in nicotine-mediated behaviors, recent evidence suggests an association between polymorphisms in the α5 nAChR gene and nicotine dependence phenotypes in humans. Thus, additional studies are imperative to elucidate the role and function of the α5 nAChR subunit in nicotine dependence. Using α5(−/−) mice, the current study aimed to examine the role of α5 nAChRs in the initial pharmacological effects of nicotine, nicotine reward using the conditioned place preference model, and the discriminative effects of nicotine using a two-lever drug discrimination model. 86Rb+ efflux and 125I-epibatidine binding assays were conducted to examine the effect of α5 nAChR subunit deletion on expression and activity of functional nAChRs. Results show that α5(−/−) mice are less sensitive to the initial effects of nicotine in antinociception, locomotor activity, and hypothermia measures and that the α5 nAChR is involved in nicotine reward. Alternatively, α5(−/−) mice did not differ from wild-type littermates in sensitivity to the discriminative stimulus effects of nicotine. Furthermore, deletion of the α5 nAChR subunit resulted in a statistically significant decrease in function in the thalamus and hindbrain, but the decreases noted in spinal cord were not statistically significant. Receptor number was unaltered in all areas tested. Taken together, results of the study suggest that α5 nAChRs are involved in nicotine-mediated behaviors relevant to development of nicotine dependence.
机译:α5烟碱乙酰胆碱受体(nAChR)亚基的掺入可以在不改变受体数量的情况下极大地影响nAChR功能。尽管很少有动物研究评估α5nAChR在尼古丁介导的行为中的作用,但最近的证据表明,α5nAChR基因的多态性与人类尼古丁依赖表型之间存在关联。因此,必须进行进一步的研究来阐明α5nAChR亚基在尼古丁依赖性中的作用和功能。本研究使用α5(-/-)小鼠,旨在研究α5nAChRs在尼古丁的初始药理作用,使用条件性位置偏爱模型的尼古丁奖赏以及使用两杠杆药物区分的尼古丁的鉴别作用中的作用。模型。进行了86Rb +外排和125I-表巴替丁结合测定,以检查α5nAChR亚基缺失对功能性nAChRs表达和活性的影响。结果表明,α5(-/-)小鼠对尼古丁在抗伤害感受,运动活动和体温过低措施方面的初始作用较不敏感,并且α5nAChR参与了尼古丁奖赏。另外,α5(-/-)小鼠与野生型同窝小鼠在对烟碱的歧视性刺激作用的敏感性方面没有差异。此外,α5nAChR亚基的缺失导致丘脑和后脑功能的统计学下降,但脊髓的下降却没有统计学意义。在所有测试区域中受体数量均未改变。两者合计,研究结果表明α5nAChRs参与尼古丁介导的行为与尼古丁依赖的发展有关。

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