可卡因使用的小鼠模型中的基因表达研究结果是否重现了人类奖赏回路可卡因使用障碍?
Do gene expression findings from mouse models of cocaine use recapitulate human cocaine use disorder in reward circuitry?
机构信息
Behavioral Genetics of Addiction Laboratory, Department of Psychology at Emory University, Atlanta, Georgia, USA.
Center for Systems Neurogenetics of Addiction, The Jackson Laboratory, Bar Harbor, Maine, USA.
出版信息
Genes Brain Behav. 2021 Feb;20(2):e12689. doi: 10.1111/gbb.12689. Epub 2020 Sep 15.
Animal models of drug use have investigated possible mechanisms governing human substance use traits for over 100 years. Most cross-species research on drug use/addiction examines behavioral overlap, but studies assessing neuromolecular (e.g. RNA) correspondence are lacking. Our study utilized transcriptome-wide data from the hippocampus and ventral tegmental area (VTA)/midbrain from a total of 35 human males with cocaine use disorder/controls and 49 male C57BL/6J cocaine/saline administering/exposed mice. We hypothesized differential expressed genes and systems of co-expressed genes (gene networks) would show appreciable overlap across mouse cocaine self-administration and human cocaine use disorder. We found modest, but significant relationships between differentially expressed genes associated with cocaine self-administration (short access) and cocaine use disorder within reward circuitry. Differentially expressed genes underlying models of acute cocaine exposure (cocaine), context re-exposure and cocaine + context re-exposure were not consistently associated with human CUD across brain regions. Investigating systems of co-expressed genes, we found several validated gene networks with weak to moderate conservation between cocaine/saline self-administering mice and disordered cocaine users/controls. The most conserved hippocampal and VTA gene networks demonstrated substantial overlap (2029 common genes) and included both novel and previously implicated targets for cocaine use/addiction. Lastly, we conducted (expression-based) phenome-wide association studies of the nine common hub genes across conserved gene networks. Common hub genes were associated with dopamine/serotonin function, cocaine self-administration and other relevant mouse traits. Overall, our study pinpointed and characterized conserved brain-related RNA patterns across mouse cocaine self-administration and human cocaine use disorder. We offer recommendations for future research and add to the dialogue surrounding pre-clinical animal research for human disease.
动物药物使用模型已经研究了可能的机制,以解释人类物质使用特征超过 100 年。大多数跨物种的药物使用/成瘾研究都检查了行为上的重叠,但缺乏评估神经分子(例如 RNA)对应关系的研究。我们的研究利用了总共 35 名可卡因使用障碍/对照男性和 49 只雄性 C57BL/6J 可卡因/盐水给药/暴露的雄性小鼠的海马体和腹侧被盖区(VTA)/中脑的转录组-wide 数据。我们假设差异表达的基因和共表达基因(基因网络)系统将在老鼠可卡因自我给药和人类可卡因使用障碍中显示出相当大的重叠。我们发现,与可卡因自我给药(短时间接触)和可卡因使用障碍相关的差异表达基因与奖励回路内的关系适度,但显著。在不同的大脑区域,可卡因急性暴露(可卡因)、情境重新暴露和可卡因+情境重新暴露模型下差异表达的基因与人类 CUD 之间没有一致的关联。研究共表达基因系统,我们发现了几个经过验证的基因网络,这些网络在可卡因/盐水自我给药的老鼠和紊乱的可卡因使用者/对照者之间存在弱到中度的保守性。最保守的海马体和 VTA 基因网络显示出很大的重叠(2029 个共同基因),包括可卡因使用/成瘾的新的和以前涉及的靶点。最后,我们对保守基因网络中的九个共同枢纽基因进行了(基于表达的)全基因组关联研究。常见的枢纽基因与多巴胺/血清素功能、可卡因自我给药和其他相关的老鼠特征有关。总的来说,我们的研究在老鼠可卡因自我给药和人类可卡因使用障碍之间确定并描述了保守的大脑相关 RNA 模式。我们为未来的研究提供了建议,并为围绕人类疾病的临床前动物研究的对话增添了内容。
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