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特定区域的中间神经元亚群在创伤相关病理和适应能力中的作用。

Region-specific involvement of interneuron subpopulations in trauma-related pathology and resilience.

机构信息

Sagol Department of Neurobiology, University of Haifa, Israel; The Integrated Brain and Behavior Research Center (IBBR), University of Haifa, Israel; Psychology Department, University of Haifa, Israel.

Department of Genetics & Molecular Neurobiology, Institute of Biology, Otto-von-Guericke-University Magdeburg, Germany.

出版信息

Neurobiol Dis. 2020 Sep;143:104974. doi: 10.1016/j.nbd.2020.104974. Epub 2020 Jun 17.

Abstract

Only a minority of trauma-exposed individuals develops Posttraumatic stress disorder (PTSD) and active processes may support trauma resilience. Individual behavioral profiling allows investigating neurobiological alterations related to resilience or pathology in animal models of PTSD and is utilized here to examine the activation of different interneuron subpopulations of the dentate gyrus-amygdala system associated with trauma resilience or pathology. To model PTSD, rats were exposed to juvenile stress combined with underwater trauma (UWT) in adulthood. Four weeks later, individual anxiety levels were assessed in the elevated plus maze test for classifying rats as highly anxious 'affected' vs. 'non-affected', i.e. behaving as control animals. Analyzing the activation of specific interneuron subpopulations in the dorsal and ventral dentate gyrus (DG), the basolateral (BLA) and central amygdala by immunohistochemical double-labeling for cFos and different interneuron markers, revealed an increased activation of cholecystokinin (CCK)-positive interneurons in the ventral DG, together with increased activation of parvalbumin- and CCK-positive interneurons in the BLA of affected trauma-exposed rats. By contrast, increased activation of neuropeptide Y (NPY)-positive interneurons was observed in the dorsal DG of trauma-exposed, but non-affected rats. To test for a direct contribution of NPY in the dorsal DG to trauma resilience, a local shRNA-mediated knock down was performed after UWT. Such a treatment significantly reduced the prevalence of resilient animals. Our results suggest that distinct interneuron populations are associated with resilience or pathology in PTSD with high regional specificity. NPY within the dorsal DG was found to significantly contribute to trauma resilience.

摘要

只有少数创伤暴露个体发展为创伤后应激障碍(PTSD),而积极的过程可能支持创伤后的适应能力。个体行为特征分析可以研究与 PTSD 动物模型中的适应能力或病理学相关的神经生物学改变,并且在这里被用于检查与适应能力或病理学相关的齿状回-杏仁核系统的不同中间神经元亚群的激活。为了模拟 PTSD,成年大鼠经历幼年期应激和水下创伤(UWT)。4 周后,通过高架十字迷宫测试评估个体焦虑水平,以将大鼠分类为高度焦虑的“受影响”与“未受影响”,即表现为对照动物。通过免疫组织化学双重标记 cFos 和不同中间神经元标志物分析背侧和腹侧齿状回(DG)、基底外侧杏仁核(BLA)和中央杏仁核中特定中间神经元亚群的激活,发现受影响的创伤暴露大鼠的 DG 腹侧的胆囊收缩素(CCK)阳性中间神经元的激活增加,同时 BLA 的副甲状腺素和 CCK 阳性中间神经元的激活增加。相比之下,在暴露于创伤但未受影响的大鼠的 DG 背侧观察到神经肽 Y(NPY)阳性中间神经元的激活增加。为了测试 NPY 在 DG 背侧对创伤适应能力的直接贡献,在 UWT 后进行局部 shRNA 介导的敲低。这种处理显著降低了适应动物的流行率。我们的结果表明,不同的中间神经元群体与 PTSD 中的适应能力或病理学有关,具有高度的区域特异性。DG 背侧的 NPY 被发现对创伤适应能力有显著贡献。

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