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产前阿片类药物暴露会重新编程对未来酒精奖励的行为反应。

Prenatal opioid exposure reprograms the behavioural response to future alcohol reward.

机构信息

Department of Pharmacology and Toxicology, Indiana University School of Medicine, Indianapolis, Indiana, USA.

Indiana University School of Medicine, Medical Scientist Training Program, Indianapolis, Indiana, USA.

出版信息

Addict Biol. 2022 Mar;27(2):e13136. doi: 10.1111/adb.13136.

Abstract

As the opioid crisis has continued to grow, so has the number of infants exposed to opioids during the prenatal period. A growing concern is that prenatal exposure to opioids may induce persistent neurological changes that increase the propensity for future addictions. Although alcohol represents the most likely addictive substance that the growing population of prenatal opioid exposed will encounter as they mature, no studies to date have examined the effect of prenatal opioid exposure on future sensitivity to alcohol reward. Using a recently developed mouse model of prenatal methadone exposure (PME), we investigated the rewarding properties of alcohol and alcohol consumption in male and female adolescent PME and prenatal saline exposed (PSE) control animals. Conditioned place preference to alcohol was disrupted in PME offspring in a sex-dependent manner with PME males exhibiting resistance to the rewarding properties of alcohol. Repeated injections of alcohol revealed enhanced sensitivity to the locomotor-stimulating effects of alcohol specific to PME females. PME males consumed significantly more alcohol over 4 weeks of alcohol access relative to PSE males and exhibited increased resistance to quinine-adulterated alcohol. Further, a novel machine learning model was developed to employ measured differences in alcohol consumption and drinking microstructure to reliably predict prenatal exposure. These findings indicate that PME alters the sensitivity to alcohol reward in adolescent mice in a sex-specific manner and suggests prenatal opioid exposure may induce persistent effects on reward neurocircuitry that can reprogram offspring behavioural response to alcohol later in life.

摘要

随着阿片类药物危机的持续加剧,产前暴露于阿片类药物的婴儿数量也在不断增加。人们越来越担心的是,产前暴露于阿片类药物可能会引起持续的神经变化,增加未来成瘾的倾向。虽然酒精是产前接触阿片类药物的不断增长的人群在成熟后最有可能接触到的成瘾物质,但迄今为止,尚无研究探讨产前阿片类药物暴露对未来对酒精奖励的敏感性的影响。使用最近开发的产前美沙酮暴露(PME)的小鼠模型,我们研究了雄性和雌性青春期 PME 和产前盐水暴露(PSE)对照动物对酒精和酒精消费的奖赏特性。条件性位置偏好到酒精在 PME 后代中以性别依赖的方式被破坏,PME 雄性表现出对酒精奖赏特性的抵抗力。重复注射酒精显示出 PME 雌性对酒精的运动刺激作用的敏感性增强。与 PSE 雄性相比,PME 雄性在 4 周的酒精摄入期间消耗的酒精明显更多,并且对奎宁掺杂的酒精表现出更高的抵抗力。此外,还开发了一种新的机器学习模型,用于利用酒精消耗和饮酒微观结构的测量差异,可靠地预测产前暴露。这些发现表明,PME 以性别特异性的方式改变了青少年小鼠对酒精奖赏的敏感性,并表明产前阿片类药物暴露可能对奖赏神经回路产生持久影响,从而改变后代对以后生活中酒精的行为反应。

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