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首页> 外文期刊>Alcoholism: Clinical and experimental research >Adolescent C57BL/6J (but not DBA/2J) mice consume greater amounts of limited-access ethanol compared to adults and display continued elevated ethanol intake into adulthood.
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Adolescent C57BL/6J (but not DBA/2J) mice consume greater amounts of limited-access ethanol compared to adults and display continued elevated ethanol intake into adulthood.

机译:与成人相比,青春期C57BL / 6J(但不是DBA / 2J)小鼠消耗更多的有限访问乙醇,并且成年后乙醇摄入量持续增加。

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BACKGROUND: Alcohol use is common during the adolescent period, a time at which a number of crucial neurobiological, hormonal, and behavioral changes occur (Spear, 2000). In order to more fully understand the complex interaction between alcohol use and these age-typical neurobiological changes, animal models must be utilized. Rodents experience a developmental period similar to that of adolescence. Although rat models have shown striking adolescent-specific differences in sensitivity to ethanol, little work has been done in mice despite the fact that the C57BL/6J (B6) and DBA2/J (D2) mice have been shown to markedly differ in ethanol preference drinking and exhibit widely different sensitivities to ethanol. METHODS: The current study examined ethanol intake in adolescent and adult B6 and D2 mice using a limited access alcohol exposure paradigm called Drinking in the Dark (DID). Additionally, the effect of adolescent (or adult) ethanol exposure on subsequent adult ethanol intake was examined by re-exposing the mice to the same paradigm once the adolescents reached adulthood. We hypothesized that adolescent (P25-45) mice would exhibit greater binge-like alcohol intake compared to adults (P60-80), and that B6 mice would exhibit greater binge-like alcohol intake compared to D2 mice. Moreover, we predicted that relative difference in binge-like alcohol intake between adolescents and adults would be greater in D2 mice. RESULTS: Adolescent B6 mice consumed more ethanol than adults in the DID model. There was no difference between adolescent and adult D2 mice. CONCLUSIONS: This work adds to the literature suggesting that adolescents will consume more ethanol than adults and that this exposure can result in altered adult intake. However, this effect seems largely dependent upon genotype. Future work will continue to examine age-related differences in ethanol intake, preference, and sensitivity in inbred mouse strains.
机译:背景:在青少年时期经常使用酒精,这时会发生许多关键的神经生物学,激素和行为改变(Spear,2000)。为了更充分地了解饮酒与这些年龄典型的神经生物学变化之间的复杂相互作用,必须使用动物模型。啮齿动物经历的发育时期与青春期相似。尽管大鼠模型对乙醇的敏感性表现出明显的青春期特异性差异,但是尽管事实证明C57BL / 6J(B6)和DBA2 / J(D2)小鼠在乙醇偏爱方面存在明显差异,但小鼠的工作却很少。饮酒并对乙醇表现出截然不同的敏感性。方法:本研究使用称为“在黑暗中饮酒”(DID)的有限接触酒精暴露范例,检查了青春期和成年B6和D2小鼠的乙醇摄入量。此外,一旦青少年达到成年期,将小鼠重新暴露于相同的范式中,即可检查青少年(或成年)乙醇暴露对随后成年乙醇摄入量的影响。我们假设,青春期(P25-45)小鼠与成人(P60-80)相比,会表现出更大的暴饮样酒精摄入量,而B6小鼠与D2小鼠相比,会表现出更大的暴饮样酒精摄入量。此外,我们预测在D2小鼠中,青少年和成年人之间的暴饮样酒精摄入量的相对差异会更大。结果:在DID模型中,青春期B6小鼠比成人消耗更多的乙醇。青春期和成年D2小鼠之间没有差异。结论:这项工作增加了文献资料,表明青少年将比成年人消耗更多的乙醇,并且这种接触会导致成年人摄入的改变。但是,这种作用似乎很大程度上取决于基因型。未来的工作将继续研究近交小鼠品系中乙醇摄入,偏好和敏感性与年龄相关的差异。

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