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衰老调节海马齿状回静息放射状胶质样干细胞在神经前体细胞刺激下被招募进入分裂的能力。

Aging Modulates the Ability of Quiescent Radial Glia-Like Stem Cells in the Hippocampal Dentate Gyrus to be Recruited into Division by Pro-neurogenic Stimuli.

机构信息

Federal Center of Brain Research and Neurotechnologies, Federal Medical Biological Agency, Moscow, 117997, Russia.

Shemyakin-Ovchinnikov Institute of Bioorganic Chemistry, Russian Academy of Sciences, Moscow, 117997, Russia.

出版信息

Mol Neurobiol. 2024 Jun;61(6):3461-3476. doi: 10.1007/s12035-023-03746-5. Epub 2023 Nov 23.

Abstract

A delicate balance between quiescence and division of the radial glia-like stem cells (RGLs) ensures continuation of adult hippocampal neurogenesis (AHN) over the lifespan. Transient or persistent perturbations of this balance due to a brain pathology, drug administration, or therapy can lead to unfavorable long-term outcomes such as premature depletion of the RGLs, decreased AHN, and cognitive deficit. Memantine, a drug used for alleviating the symptoms of Alzheimer's disease, and electroconvulsive seizure (ECS), a procedure used for treating drug-resistant major depression or bipolar disorder, are known strong AHN inducers; they were earlier demonstrated to increase numbers of dividing RGLs. Here, we demonstrated that 1-month stimulation of quiescent RGLs by either memantine or ECS leads to premature exhaustion of their pool and altered AHN at later stages of life and that aging of the brain modulates the ability of the quiescent RGLs to be recruited into the cell cycle by these AHN inducers. Our findings support the aging-related divergence of functional features of quiescent RGLs and have a number of implications for the practical assessment of drugs and treatments with respect to their action on quiescent RGLs at different stages of life in animal preclinical studies.

摘要

静止和分裂的放射状胶质样干细胞(RGLs)之间的微妙平衡确保了成年海马神经发生(AHN)在整个生命周期内的持续进行。由于脑病理学、药物治疗或治疗导致这种平衡的短暂或持久破坏,可能导致不利的长期后果,如 RGL 的过早耗竭、AHN 减少和认知缺陷。美金刚,一种用于缓解阿尔茨海默病症状的药物,以及电惊厥(ECS),一种用于治疗抗药性重度抑郁症或双相情感障碍的程序,已知是强烈的 AHN 诱导剂;它们之前被证明可以增加分裂的 RGL 的数量。在这里,我们证明了无论是美金刚还是 ECS,对静止的 RGL 进行为期 1 个月的刺激会导致其池过早耗尽,并在生命后期改变 AHN,而大脑的衰老会调节静止的 RGL 被这些 AHN 诱导剂招募到细胞周期的能力。我们的发现支持与衰老相关的静止 RGL 功能特征的发散,并对在动物临床前研究中,在不同生命阶段评估药物和治疗方法对静止 RGL 的作用具有重要意义。

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