恐惧记忆的分子印迹:双链DNA损伤在创伤后应激障碍中的潜在机制探讨OA
Molecular imprinting of fear memory:mechanisms and therapeutic prospects of DNA damage in post-traumatic stress disorder
创伤后应激障碍(PTSD)是个体经历重大创伤事件后罹患的慢性焦虑障碍,其特征为恐惧记忆的过度泛化,自发唤起与消退障碍.研究发现,神经元生理活动诱导的DNA损伤不仅参与恐惧记忆的形成与巩固,而且其修复通路的异常极有可能与PTSD病理机制密切相关.该文综述了神经元DNA损伤的生理来源、分子机制及其生理意义,重点探讨了DNA双链断裂(DSB)在恐惧记忆的形成和维持中可能存在的调控作用及其作为恐惧记忆分子印迹的潜在机制,并进一步展望靶向DNA损伤修复通路在PTSD治疗中的转化潜力,可为发展新型PTSD治疗药物提供参考.
Post-traumatic stress disorder(PTSD)is a chronic anxiety disorder that occurs after an individual experienc-es a major traumatic event,characterized by the overgeneralization of fear memory,spontaneous retrieval,and impaired extinction.Recent studies have revealed that neuronal activity-induced DNA damage is not only involved in the formation and consolidation of fear memory,but also closely associated with the pathological mechanisms of PTSD due to abnormalities in its repair pathways.This review summarizes the physiological sources,molecular mechanisms,and physiological significance of neuronal DNA damage in general and the potential regulatory role of DNA double-strand breaks(DSBs)in the formation and maintenance of fear memory in particular.It also explores the underlying mechanisms by which DSBs may serve as molecular imprints of fear memory.This review also predicts the translational potential of targeting DNA damage repair pathways in PTSD treatment in the hope of providing data for developing novel therapeutic drugs for PTSD.
付文亮;高波;张超
军事科学院军事医学研究院,北京 100850军事科学院军事医学研究院,北京 100850军事科学院军事医学研究院,北京 100850
生物科学
DNA损伤恐惧记忆创伤后应激障碍DNA修复
DNA damagefear memorypost-traumatic stress disorderDNA repair
《军事医学》 2026 (5)
381-385,5
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