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青春期小鼠同时接触尼古丁和乙醇,对接触期间、短期和长期戒断期间的焦虑水平有不同影响。

Combined exposure to nicotine and ethanol in adolescent mice differentially affects anxiety levels during exposure, short-term, and long-term withdrawal.

作者信息

Abreu-Villaça Yael, Nunes Fernanda, do E Queiroz-Gomes Fabíola, Manhães Alex C, Filgueiras Cláudio C

机构信息

Laboratório de Neurofisiologia, Departamento de Ciências Fisiológicas, Instituto de Biologia Roberto Alcântara Gomes, Centro Biomédico, Universidade do Estado do Rio de Janeiro, Rio de Janeiro, Brazil.

出版信息

Neuropsychopharmacology. 2008 Feb;33(3):599-610. doi: 10.1038/sj.npp.1301429. Epub 2007 Apr 25.

Abstract

Smoking and consumption of alcoholic beverages are frequently associated during adolescence. This association could be explained by the cumulative behavioral effects of nicotine and ethanol, particularly those related to anxiety levels. However, despite epidemiological findings, there have been few animal studies of the basic neurobiology of the combined exposure in the adolescent brain. In the present work we assessed, through the use of the elevated plus maze, the short- and long-term anxiety effects of nicotine (NIC) and/or ethanol (ETOH) exposure during adolescence (from the 30th to the 45th postnatal day) in four groups of male and female C57BL/6 mice: (1) Concomitant NIC (nicotine free-base solution (50 microg/ml) in 2% saccharin to drink) and ETOH (ethanol solution (25%, 2 g/kg) i.p. injected every other day) exposure; (2) NIC exposure; (3) ETOH exposure; (4) Vehicle. C57BL/6 mice were selected, in spite of the fact that they present slower ethanol metabolism, because they readily consume nicotine in the concentration used in the present study. During exposure (45th postnatal day: PN45), our results indicated that ethanol was anxiolytic in adolescent mice and that nicotine reverted this effect. Short-term drug withdrawal (PN50) elicited sex-dependent effects: exposure to nicotine and/or ethanol was anxiogenic only for females. Although neither nicotine nor ethanol effects persisted up to 1 month postexposure (PN75), the coadministration elicited an anxiogenic response. In spite of the fact that generalizations based on the results from a single strain of mice are prone to shortcomings, our results suggest that the deficient response to the anxiolytic effects of ethanol in adolescents co-exposed to nicotine may drive higher ethanol consumption. Additionally, increased anxiety during long-term smoking and drinking withdrawal may facilitate relapse to drug use.

摘要

在青少年时期,吸烟与酒精饮料的消费常常同时出现。这种关联可以通过尼古丁和乙醇的累积行为效应来解释,尤其是那些与焦虑水平相关的效应。然而,尽管有流行病学研究结果,但关于青少年大脑中联合暴露的基础神经生物学的动物研究却很少。在本研究中,我们通过使用高架十字迷宫,评估了四组雄性和雌性C57BL/6小鼠在青春期(出生后第30天至第45天)暴露于尼古丁(NIC)和/或乙醇(ETOH)后的短期和长期焦虑效应:(1)同时暴露于NIC(饮用含2%糖精的尼古丁游离碱溶液(50微克/毫升))和ETOH(每隔一天腹腔注射25%乙醇溶液(2克/千克));(2)暴露于NIC;(3)暴露于ETOH;(4)给予溶剂。尽管C57BL/6小鼠的乙醇代谢较慢,但仍选择它们,因为它们能轻易消耗本研究中使用浓度的尼古丁。在暴露期间(出生后第45天:PN45),我们的结果表明,乙醇对青春期小鼠具有抗焦虑作用,而尼古丁则逆转了这种作用。短期停药(PN50)产生了性别依赖性效应:暴露于尼古丁和/或乙醇仅对雌性具有致焦虑作用。尽管暴露后1个月(PN75)时尼古丁和乙醇的效应均未持续存在,但联合给药引发了致焦虑反应。尽管基于单一品系小鼠的结果进行概括容易存在缺陷,但我们的结果表明,同时暴露于尼古丁的青少年对乙醇抗焦虑作用的反应不足可能导致更高的乙醇消费量。此外,长期吸烟和饮酒戒断期间焦虑增加可能会促进药物使用的复发。

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