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产前雄激素受体激活以性别特异性的方式决定成年期的酒精和水摄入。

Prenatal androgen receptor activation determines adult alcohol and water drinking in a sex-specific way.

机构信息

Department of Psychiatry and Psychotherapy, University Clinic, Friedrich-Alexander-University Erlangen-Nuremberg, Germany.

Department of Nephrology and Hypertension, Friedrich-Alexander-University Erlangen-Nuremberg, Germany.

出版信息

Addict Biol. 2018 May;23(3):904-920. doi: 10.1111/adb.12540. Epub 2017 Aug 4.

Abstract

Alcohol use disorders are major psychiatric disorders. Correlational studies in humans suggested organizational hormonal effects during embryonic development as a risk factor for adult alcohol dependence. Permanent changes can be induced by the activity of sex hormones, like testosterone. Here, we demonstrate a relationship between prenatal androgen receptor (AR)-activation and adult alcohol as well as water drinking in mice in a sex-dependent fashion. Prenatal AR inhibition using the antagonist flutamide decreased adult male alcohol consumption. In contrast, prenatal AR activation by dihydrotestosterone (DHT) led to an increase in adult alcohol consumption in females. These effects were different in adult water drinking, flutamide increased water consumption in females and DHT increased water consumption in males. Prenatal flutamide reduced locomotion and anxiety in adult males but was ineffective in females. We found that prenatal AR activation controls adult levels of monoaminergic modulatory transmitters in the brain and blood hormone levels in a sex-specific way. RNA-Seq analysis confirmed a prenatal AR mediated control of adult expression of alcohol drinking-related genes like Bdnf and Per2. These findings demonstrate that prenatal androgen activity is a risk factor for the establishment of alcohol consumption in adults by its organizational effects.

摘要

酒精使用障碍是一种主要的精神疾病。人类的相关性研究表明,胚胎发育过程中的组织激素效应是成年酒精依赖的一个风险因素。性荷尔蒙的活动可以诱导永久性的变化,比如睾丸激素。在这里,我们以性别依赖的方式证明了小鼠产前雄激素受体(AR)激活与成年酒精和水摄入之间的关系。使用拮抗剂氟他胺抑制产前 AR 可减少成年雄性的酒精摄入量。相比之下,产前 DHT(二氢睾酮)激活导致雌性成年酒精摄入量增加。这些影响在成年水摄入中有所不同,氟他胺增加了雌性的水摄入量,而 DHT 增加了雄性的水摄入量。产前氟他胺减少了成年雄性的运动和焦虑,但对雌性无效。我们发现,产前 AR 激活以性别特异性的方式控制大脑和血液激素水平中的单胺能调节递质的成年水平。RNA-Seq 分析证实,产前 AR 介导了与酒精摄入相关的基因如 Bdnf 和 Per2 的成年表达的控制。这些发现表明,产前雄激素活性是通过其组织效应成为成年酒精摄入的一个风险因素。

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