Stress-enhanced ethanol drinking does not increase sensitivity to the effects of a CRF-R1 antagonist on ethanol intake in male and female mice

IF 2.5 4区医学 Q3 PHARMACOLOGY & PHARMACY

Alcohol Pub Date : 2024-01-05 DOI:10.1016/j.alcohol.2024.01.001

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Abstract

Research confirms that stress is associated with alcohol drinking and relapse in males and females and that there are sex differences in the alcohol-related adaptations of stress pathways. The predator stress (PS) model of traumatic stress produces an increase in alcohol drinking or self-administration in a subpopulation of rodents, so it is utilized as an animal model of comorbid alcohol use disorder (AUD) and post-traumatic stress disorder (PTSD). Previous work determined that sensitivity to PS-enhanced drinking produced sex differences in proteins related to stress-regulating systems in the medial prefrontal cortex and hippocampus. The present studies examined whether male and female C57BL/6J mice differ in sensitivity to the ability of the corticotropin releasing factor receptor 1 antagonist CP-376395 to decrease PS-enhanced drinking. In control studies, CP-376395 doses of 5, 10, and 20 mg/kg dose-dependently decreased 4-h ethanol drinking. Next, CP-376395 doses of 5 and 10 mg/kg were tested for effects on ethanol drinking in mice with differential sensitivity to PS-enhanced drinking. Subgroups of “Sensitive” and “Resilient” male and female mice were identified based on changes in ethanol intake in an unrestricted-access ethanol-drinking procedure following four exposures to PS (dirty rat bedding). During the first 2 h post-injection of CP-376395, both doses significantly decreased ethanol licks versus vehicle in the females, with no significant interaction between subgroups, whereas the 10 mg/kg dose significantly decreased ethanol licks versus vehicle in the “Resilient” males. Thus, sensitivity to the suppressive effect of CP-376395 on stress-induced ethanol intake was greater in females versus males, whereas sensitivity and resilience to PS-enhanced drinking produced differential sensitivity to the ability of CP-376395 to decrease ethanol drinking only in male mice. Our results argue against greater efficacy of CRF-R1's ability to decrease ethanol intake in subjects with traumatic stress-enhanced ethanol drinking.

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应激增强型乙醇饮用不会提高雌雄小鼠对 CRF-R1 拮抗剂影响乙醇摄入量的敏感性

研究证实，应激与男性和女性的饮酒和复酒有关，应激途径中与酒精相关的适应性存在性别差异。捕食者应激（PS）创伤应激模型在啮齿动物亚群中会产生饮酒或自我给药的增加，因此被用作合并酒精使用障碍（AUD）和创伤后应激障碍（PTSD）的动物模型。之前的研究发现，对 PS 增强型饮酒的敏感性会导致内侧前额叶皮层和海马中与压力调节系统相关的蛋白质出现性别差异。本研究考察了雌雄 C57BL/6J 小鼠对促肾上腺皮质激素释放因子受体 1 拮抗剂 CP-376395 降低 PS 增强饮酒能力的敏感性是否存在差异。在对照研究中，CP-376395 的剂量为 5、10 和 20 毫克/千克，其剂量依赖性降低了 4 小时的乙醇饮酒量。接下来，CP-376395 的 5 和 10 毫克/千克剂量被用于测试对 PS 增强饮酒敏感性不同的小鼠的乙醇饮酒影响。根据四次接触 PS（肮脏的大鼠垫料）后在无限制接触乙醇饮用程序中乙醇摄入量的变化，确定了 "敏感 "和 "复原 "雄性和雌性小鼠亚组。在注射 CP-376395 后的最初 2 小时内，雌性小鼠的乙醇舔食量与车辆相比均显著减少，亚组之间无显著交互作用，而 "抗逆性 "雄性小鼠的乙醇舔食量与车辆相比，10 毫克/千克剂量显著减少。因此，雌性小鼠对 CP-376395 对应激诱导的乙醇摄入的抑制作用更敏感，而雄性小鼠对 PS 增强的饮酒的敏感性和恢复力则不同，只有雄性小鼠对 CP-376395 减少乙醇饮酒的能力更敏感。我们的研究结果表明，CRF-R1在创伤应激增强乙醇摄入的受试者中具有更强的降低乙醇摄入量的功效。

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来源期刊

Alcohol 医学-毒理学

CiteScore

4.60

自引率

4.30%

发文量

审稿时长

15.6 weeks

期刊介绍： Alcohol is an international, peer-reviewed journal that is devoted to publishing multi-disciplinary biomedical research on all aspects of the actions or effects of alcohol on the nervous system or on other organ systems. Emphasis is given to studies into the causes and consequences of alcohol abuse and alcoholism, and biomedical aspects of diagnosis, etiology, treatment or prevention of alcohol-related health effects. Intended for both research scientists and practicing clinicians, the journal publishes original research on the neurobiological, neurobehavioral, and pathophysiological processes associated with alcohol drinking, alcohol abuse, alcohol-seeking behavior, tolerance, dependence, withdrawal, protracted abstinence, and relapse. In addition, the journal reports studies on the effects alcohol on brain mechanisms of neuroplasticity over the life span, biological factors associated with adolescent alcohol abuse, pharmacotherapeutic strategies in the treatment of alcoholism, biological and biochemical markers of alcohol abuse and alcoholism, pathological effects of uncontrolled drinking, biomedical and molecular factors in the effects on liver, immune system, and other organ systems, and biomedical aspects of fetal alcohol spectrum disorder including mechanisms of damage, diagnosis and early detection, treatment, and prevention. Articles are published from all levels of biomedical inquiry, including the following: molecular and cellular studies of alcohol''s actions in vitro and in vivo; animal model studies of genetic, pharmacological, behavioral, developmental or pathophysiological aspects of alcohol; human studies of genetic, behavioral, cognitive, neuroimaging, or pathological aspects of alcohol drinking; clinical studies of diagnosis (including dual diagnosis), treatment, prevention, and epidemiology. The journal will publish 9 issues per year; the accepted abbreviation for Alcohol for bibliographic citation is Alcohol.