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首页> 外文期刊>Alcoholism: Clinical and experimental research >The selectively bred high alcohol sensitivity (HAS) and low alcohol sensitivity (LAS) rats differ in sensitivity to nicotine.
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The selectively bred high alcohol sensitivity (HAS) and low alcohol sensitivity (LAS) rats differ in sensitivity to nicotine.

机译:选择性饲养的高酒精敏感性(HAS)和低酒精敏感性(LAS)大鼠对尼古丁的敏感性不同。

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摘要

BACKGROUND: Studies in rodents selectively bred to differ in alcohol sensitivity have suggested that nicotine and ethanol sensitivities may cosegregate during selective breeding. This suggests that ethanol and nicotine sensitivities may in part be genetically correlated. METHODS: Male and female high alcohol sensitivity (HAS), control alcohol sensitivity, and low alcohol sensitivity (LAS) rats were tested for nicotine-induced alterations in locomotor activity, body temperature, and seizure activity. Plasma and brain levels of nicotine and its primary metabolite, cotinine, were measured in these animals, as was the binding of [3H]cytisine, [3H]epibatidine, and [125I]alpha-bungarotoxin in eight brain regions. RESULTS: Both replicate HAS lines were more sensitive to nicotine-induced locomotor activity depression than the replicate LAS lines. No consistent HAS/LAS differences were seen on other measures of nicotine sensitivity; however, females were more susceptible to nicotine-induced seizures than males. No HAS/LAS differences in nicotine or cotinine levels were seen, nor were differences seen in the binding of nicotinic ligands. Females had higher levels of plasma cotinine and brain nicotine than males but had lower brain cotinine levels than males. CONCLUSIONS: Sensitivity to a specific action of nicotine cosegregates during selective breeding for differential sensitivity to a specific action of ethanol. The differential sensitivity of the HAS/LAS rats is due to differences in central nervous system sensitivity and not to pharmacokinetic differences. The differential central nervous system sensitivity cannot be explained by differences in the numbers of nicotinic receptors labeled in ligand-binding experiments. The apparent genetic correlation between ethanol and nicotine sensitivities suggests that common genes modulate, in part, the actions of both ethanol and nicotine and may explain the frequent coabuse of these agents.
机译:背景:对选择性饲养以具有不同酒精敏感性的啮齿动物的研究表明,尼古丁和乙醇的敏感性可能在选择性育种过程中同时分离。这表明乙醇和尼古丁的敏感性可能部分与遗传相关。方法:对雄性和雌性高酒精敏感度(HAS),对照酒精敏感度和低酒精敏感度(LAS)大鼠进行了尼古丁诱导的运动能力,体温和癫痫发作改变的测试。在这些动物中测量了尼古丁及其主要代谢产物可替宁的血浆和脑水平,以及在八个大脑区域中的[3H]胱氨酸,[3H]表巴替丁和[125I]α-真菌毒素的结合。结果:两个复制的HAS系比复制的LAS系对尼古丁引起的自发活动抑制更敏感。在其他尼古丁敏感性测量中,未观察到一致的HAS / LAS差异。但是,女性比男性更容易受到尼古丁引起的癫痫发作的影响。没有观察到烟碱或可替宁水平的HAS / LAS差异,也没有观察到烟碱配体结合的差异。女性的血浆可替宁和大脑尼古丁水平高于男性,但脑可替宁水平却低于男性。结论:在选择性育种中对尼古丁共偏析的特定作用的敏感性,对乙醇的特定作用的敏感性不同。 HAS / LAS大鼠的敏感性差异是由于中枢神经系统敏感性差异而不是药代动力学差异所致。中枢神经系统敏感性的差异不能通过配体结合实验中标记的烟碱样受体数量的差异来解释。乙醇和尼古丁敏感性之间的明显遗传相关性表明,共同基因部分地调节了乙醇和尼古丁的作用,并可能解释了这些药物的频繁滥用。

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