Synaptic remodeling of GluA1 and GluA2 expression in the nucleus accumbens promotes susceptibility to cognitive deficits concomitant with downstream GSK3β mediated neurotoxicity in female mice during abstinence from voluntary oral methamphetamine

Addiction neuroscience Pub Date : 2023-06-16 DOI:10.1016/j.addicn.2023.100112

Nicoletta Memos , Jorge A. Avila , Edgar Rodriguez , Peter A. Serrano

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Abstract

Stimulant-use disorders can present with long-term cognitive and mental health deficits. Little is known about the underlying molecular mechanisms perpetuating sex differences in cognitive and behavioral deficits in preclinical models of addiction to stimulants such as methamphetamine (MA). The current study investigated the neurochemical shifts underlying sex disparities in MA-induced working memory deficits and an addictive phenotype following abstinence from chronic MA abuse. We used our previously reported mouse model of voluntary oral methamphetamine administration (VOMA) consisting of an acquisition phase (days 1–14) characterized by escalating doses of MA and a binge phase (days 14–28) characterized by static doses. Female VOMA mice exhibited sustained MA consumption during the binge phase, demonstrating sex-specific vulnerabilities to the maintenance of MA addiction. The 8-arm radial maze was used to test spatial working memory performance following abstinence from VOMA. Results indicate working memory deficits correlated to higher MA consumption in females only. Hippocampal and accumbal tissue were collected and analyzed by immunoblotting. Female VOMA mice had decreased GluA1, but not GluA2, in the hippocampus, which may perpetuate synaptic destabilization and working memory deficits. Female-specific increases in GluA1 and p-GSK3β expression in accumbal tissue suggest vulnerability toward abstinence-induced drug craving and heightened downstream neurotoxicity. Our study reveals female-specific neurochemical shifts in hippocampal and accumbal AMPA receptor signaling following abstinence from chronic MA consumption that may perpetuate female susceptibility to MA-induced cognitive deficits. These data demonstrate a novel molecular pathway that would exacerbate memory deficits and perpetuate an addictive phenotype in female populations following MA abuse.

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在雌性小鼠自愿口服甲基苯丙胺戒断期间，伏隔核中GluA1和GluA2表达的突触重塑促进了认知缺陷伴随下游GSK3β介导的神经毒性的易感性

兴奋剂使用障碍可表现为长期的认知和精神健康缺陷。对于甲基苯丙胺(MA)等兴奋剂成瘾的临床前模型中导致认知和行为缺陷性别差异的潜在分子机制，我们知之甚少。目前的研究调查了MA诱导的工作记忆缺陷和慢性MA滥用戒断后的成瘾表型的性别差异背后的神经化学变化。我们使用了先前报道的自愿口服甲基苯丙胺小鼠模型(VOMA)，该模型包括以MA剂量递增为特征的获取阶段(1-14天)和以静态剂量为特征的暴食阶段(14-28天)。雌性VOMA小鼠在暴食期表现出持续的MA消耗，显示出对MA成瘾维持的性别特异性脆弱性。采用八臂径向迷宫测试戒断VOMA后的空间工作记忆表现。结果表明，工作记忆缺陷仅与女性较高的MA消耗相关。收集海马和伏隔区组织，进行免疫印迹分析。雌性VOMA小鼠海马体中的GluA1减少，但GluA2没有减少，这可能使突触不稳定和工作记忆缺陷长期存在。女性伏隔组织中GluA1和p-GSK3β表达的特异性增加表明，她们容易受到戒断引起的药物渴求和下游神经毒性的影响。我们的研究揭示了女性特异性的海马和伏隔区AMPA受体信号的神经化学变化，这可能使女性对MA诱导的认知缺陷的易感性永续存在。这些数据证明了一种新的分子途径会加剧记忆缺陷，并使女性滥用MA后的成瘾表型永续存在。

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