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产前乙醇暴露会改变成年雄性小鼠后代对单独给予阿扑吗啡以及阿扑吗啡与乙醇联合给予时对运动活动影响的敏感性。

Prenatal ethanol exposure alters sensitivity to the effects of apomorphine given alone and in combination with ethanol on locomotor activity in adult male mouse offspring.

作者信息

Becker H C, Weathersby R T, Hale R L

机构信息

VA Medical Center, Research Service, Charleston, SC 29401.

出版信息

Neurotoxicol Teratol. 1995 Jan-Feb;17(1):57-64. doi: 10.1016/0892-0362(94)00055-i.

DOI:10.1016/0892-0362(94)00055-i
PMID:7708020
Abstract

Previous studies have indicated that prenatal ethanol (EtOH) exposure alters developing catecholamine (CA) systems and acute sensitivity to the locomotor stimulant effects of EtOH. The purpose of this study was to examine whether prenatal EtOH exposure influences the effects of the direct dopamine (DA) agonist apomorphine given alone as well as in combination with a low-dose stimulant challenge of EtOH. Standard lab chow or liquid diets containing either 25% EtOH-derived calories (EDC), or 0% EDC were given to pregnant C3H/He mice on gestation days 6-18. At 90 days of age, male offspring from each prenatal treatment group were monitored for 10 min in an open field following IP injections of apomorphine (0, 0.15, 0.3, 0.6, or 1.2 mg/kg) and either EtOH (1.5 g/kg) or saline. EtOH alone increased activity by 120-143% in all three groups of offspring. In control offspring, apomorphine dose-dependently decreased activity up to 74%-78% and blocked the stimulant effect of EtOH at all doses tested. However, in prenatal EtOH-exposed offspring, higher doses of apomorphine were significantly less effective in reducing both baseline and EtOH-stimulated activity compared to control mice. This effect is most likely not due to differences in pharmacokinetics, because blood EtOH concentrations were similar across apomorphine doses and prenatal treatment conditions. As such, these results support the hypothesis that prenatal exposure to EtOH alters acute sensitivity to the locomotor stimulant effects of EtOH, particularly under conditions in which CA systems mediating those effects are additionally challenged. In addition, the results suggest that prenatal EtOH exposure results in a long-lasting perturbation of central DA receptor sensitivity.

摘要

先前的研究表明,产前乙醇(EtOH)暴露会改变发育中的儿茶酚胺(CA)系统以及对EtOH运动刺激作用的急性敏感性。本研究的目的是检验产前EtOH暴露是否会影响单独给予直接多巴胺(DA)激动剂阿扑吗啡以及与低剂量EtOH刺激挑战联合使用时的效果。在妊娠第6 - 18天,给怀孕的C3H/He小鼠喂食标准实验室饲料或含有25%乙醇衍生热量(EDC)或0% EDC的液体饮食。在90日龄时,对每个产前治疗组的雄性后代腹腔注射阿扑吗啡(0、0.15、0.3、0.6或1.2 mg/kg)以及EtOH(1.5 g/kg)或生理盐水后,在旷场中监测10分钟。单独使用EtOH可使所有三组后代的活动增加120% - 143%。在对照后代中,阿扑吗啡剂量依赖性地使活动减少高达74% - 78%,并在所有测试剂量下阻断了EtOH的刺激作用。然而,与对照小鼠相比,在产前暴露于EtOH的后代中,较高剂量的阿扑吗啡在降低基线和EtOH刺激的活动方面明显效果较差。这种效应很可能不是由于药代动力学差异,因为在不同阿扑吗啡剂量和产前治疗条件下,血液EtOH浓度相似。因此,这些结果支持以下假设:产前暴露于EtOH会改变对EtOH运动刺激作用的急性敏感性,特别是在介导这些作用的CA系统受到额外挑战的情况下。此外,结果表明产前EtOH暴露会导致中枢DA受体敏感性的长期扰动。

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