Distinct Chrna5 mutations link excessive alcohol use to types I/II vulnerability profiles and IPN GABAergic neurons.

IF 5.8 1区 医学 Q1 PSYCHIATRY Translational Psychiatry Pub Date : 2024-11-06 DOI:10.1038/s41398-024-03164-8
Léa Tochon, Nadia Henkous, Morgane Besson, Uwe Maskos, Vincent David
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Abstract

Genome wide association and animal studies have implicated genetic variations in CHRNΑ5, encoding the α5 subunit-containing nicotinic acetylcholine receptors (α5*nAChRs), as a risk factor for developing alcohol use disorders (AUDs). To understand how α5*nAChR mutations may influence alcohol (EtOH) drinking behavior, we used a two-bottle choice procedure with intermittent access to alcohol in male and female transgenic mice expressing either the highly frequent human single nucleotide polymorphism (α5SNP/rs16969968) or a deletion of the Chrna5 gene (α5KO). AUDs-related preconsommatory traits (anxiety, sensation-seeking and impulsivity) were assessed with a battery of relevant tasks (elevated-plus maze, novel place preference and step-down inhibitory avoidance). The implication of the α5-expressing IPN GABAergic neurons in AUDs and related behavioral traits was verified using neurospecific lentiviral (LV)-induced reexpression of the α5 subunit in α5KOxGAD-Cre mice. Both α5SNP and α5KO mice showed over-consumption of EtOH, but displayed opposite vulnerability profiles consistent with Cloninger's subtypes of human AUDs. α5SNP mice showed Type I-like characteristics, i.e., high anxiety, novelty avoidance, whereas α5KOs exhibited Type II-like features such as low anxiety and high impulsivity. LV re-expression of the α5 subunit in IPN GABAergic neurons restored the control of EtOH intake and improved the impulsive phenotype. We demonstrate that the SNP (rs16969968) or null mutation of Chrna5 result in increased volitional EtOH consumption but opposite effects on anxiety, novelty-seeking and impulsive-like behaviors that match Cloninger type I and II of AUDs, including sex-related variations. IPN GABAergic neurons expressing α5*nAChRs play a key role in limiting both EtOH drinking and motor impulsivity.

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不同的 Chrna5 基因突变将过度饮酒与 I/II 型易损性特征和 IPN GABA 能神经元联系起来。
全基因组关联和动物研究表明,编码含α5亚基的烟碱乙酰胆碱受体(α5*nAChRs)的CHRNΑ5基因变异是罹患酒精使用障碍(AUDs)的一个危险因素。为了了解α5*nAChR突变如何影响饮酒(EtOH)行为,我们在表达高频人类单核苷酸多态性(α5SNP/rs16969968)或Chrna5基因缺失(α5KO)的雄性和雌性转基因小鼠中采用了间歇性获取酒精的双瓶选择程序。通过一系列相关任务(高架迷宫、新奇场所偏好和降阶抑制性回避)评估了与 AUD 相关的前认知特征(焦虑、感觉寻求和冲动)。利用神经特异性慢病毒(LV)诱导α5亚基在α5KOxGAD-Cre小鼠中的再表达,验证了表达α5的IPN GABA能神经元对AUDs和相关行为特征的影响。α5SNP和α5KO小鼠都表现出过度摄入乙醇,但表现出与克隆宁格的人类AUD亚型一致的相反的易感性特征。α5SNP小鼠表现出类似I型的特征,即高度焦虑、回避新事物,而α5KOs则表现出类似II型的特征,如低焦虑和高冲动性。在 IPN GABA 能神经元中 LV 重表达 α5 亚基可恢复对乙醇摄入的控制并改善冲动表型。我们证明,Chrna5的SNP(rs16969968)或无效突变会导致EtOH的自愿消耗量增加,但对焦虑、寻求新奇和冲动行为的影响却相反,这与AUD的Cloninger I型和II型相匹配,包括与性别相关的变异。表达α5*nAChRs的IPN GABA能神经元在限制EtOH饮酒和运动冲动方面起着关键作用。
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来源期刊
CiteScore
11.50
自引率
2.90%
发文量
484
审稿时长
23 weeks
期刊介绍: Psychiatry has suffered tremendously by the limited translational pipeline. Nobel laureate Julius Axelrod''s discovery in 1961 of monoamine reuptake by pre-synaptic neurons still forms the basis of contemporary antidepressant treatment. There is a grievous gap between the explosion of knowledge in neuroscience and conceptually novel treatments for our patients. Translational Psychiatry bridges this gap by fostering and highlighting the pathway from discovery to clinical applications, healthcare and global health. We view translation broadly as the full spectrum of work that marks the pathway from discovery to global health, inclusive. The steps of translation that are within the scope of Translational Psychiatry include (i) fundamental discovery, (ii) bench to bedside, (iii) bedside to clinical applications (clinical trials), (iv) translation to policy and health care guidelines, (v) assessment of health policy and usage, and (vi) global health. All areas of medical research, including — but not restricted to — molecular biology, genetics, pharmacology, imaging and epidemiology are welcome as they contribute to enhance the field of translational psychiatry.
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