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个体的应激脆弱性可由海马体中的短期记忆和 AMPA 受体亚基比率预测。

Individual stress vulnerability is predicted by short-term memory and AMPA receptor subunit ratio in the hippocampus.

机构信息

Research Group Neurobiology of Stress, Max Planck Institute of Psychiatry, 80804 Munich, Germany.

出版信息

J Neurosci. 2010 Dec 15;30(50):16949-58. doi: 10.1523/JNEUROSCI.4668-10.2010.

Abstract

Increased vulnerability to aversive experiences is one of the main risk factors for stress-related psychiatric disorders as major depression. However, the molecular bases of vulnerability, on the one hand, and stress resilience, on the other hand, are still not understood. Increasing clinical and preclinical evidence suggests a central involvement of the glutamatergic system in the pathogenesis of major depression. Using a mouse paradigm, modeling increased stress vulnerability and depression-like symptoms in a genetically diverse outbred strain, and we tested the hypothesis that differences in AMPA receptor function may be linked to individual variations in stress vulnerability. Vulnerable and resilient animals differed significantly in their dorsal hippocampal AMPA receptor expression and AMPA receptor binding. Treatment with an AMPA receptor potentiator during the stress exposure prevented the lasting effects of chronic social stress exposure on physiological, neuroendocrine, and behavioral parameters. In addition, spatial short-term memory, an AMPA receptor-dependent behavior, was found to be predictive of individual stress vulnerability and response to AMPA potentiator treatment. Finally, we provide evidence that genetic variations in the AMPA receptor subunit GluR1 are linked to the vulnerable phenotype. Therefore, we propose genetic variations in the AMPA receptor system to shape individual stress vulnerability. Those individual differences can be predicted by the assessment of short-term memory, thereby opening up the possibility for a specific treatment by enhancing AMPA receptor function.

摘要

易感性增加对不愉快的体验是与压力相关的精神疾病的主要风险因素之一,如重度抑郁症。然而,易感性的分子基础,一方面,和压力弹性,另一方面,仍然不被理解。越来越多的临床前和临床证据表明,谷氨酸能系统在重度抑郁症的发病机制中起核心作用。我们使用一种模拟遗传多样化的近交系中压力易感性增加和类似抑郁症状的小鼠模型,检验了 AMPA 受体功能差异可能与个体压力易感性差异有关的假设。易感性和弹性动物在其背侧海马 AMPA 受体表达和 AMPA 受体结合方面存在显著差异。在应激暴露期间用 AMPA 受体增强剂治疗可以防止慢性社会应激暴露对生理、神经内分泌和行为参数的持久影响。此外,空间短期记忆,一种依赖于 AMPA 受体的行为,被发现与个体压力易感性和对 AMPA 增强剂治疗的反应有关。最后,我们提供了证据表明,AMPA 受体亚基 GluR1 的遗传变异与易感性表型有关。因此,我们提出 AMPA 受体系统的遗传变异来塑造个体的压力易感性。通过评估短期记忆可以预测这些个体差异,从而通过增强 AMPA 受体功能来实现特定的治疗。

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