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衰老海马中新颗粒细胞的高可塑性。

High Plasticity of New Granule Cells in the Aging Hippocampus.

机构信息

Laboratorio de Plasticidad Neuronal, Fundación Instituto Leloir, Instituto de Investigaciones Bioquímicas de Buenos Aires, Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Av. Patricias Argentinas 435, Buenos Aires C1405BWE, Argentina.

División de Neurociencia Celular y Molecular, Instituto de Biología Celular y Neurociencias (IBCN-CONICET-UBA), Facultad de Medicina, Paraguay 2155, Buenos Aires C1121ABG, Argentina.

出版信息

Cell Rep. 2017 Oct 31;21(5):1129-1139. doi: 10.1016/j.celrep.2017.09.064.

Abstract

During aging, the brain undergoes changes that impair cognitive capacity and circuit plasticity, including a marked decrease in production of adult-born hippocampal neurons. It is unclear whether development and integration of those new neurons are also affected by age. Here, we show that adult-born granule cells (GCs) in aging mice are scarce and exhibit slow development, but they display a remarkable potential for structural plasticity. Retrovirally labeled 3-week-old GCs in middle-aged mice were small, underdeveloped, and disconnected. Neuronal development and integration were accelerated by voluntary exercise or environmental enrichment. Similar effects were observed via knockdown of Lrig1, an endogenous negative modulator of neurotrophin receptors. Consistently, blocking neurotrophin signaling by Lrig1 overexpression abolished the positive effects of exercise. These results demonstrate an unparalleled degree of plasticity in the aging brain mediated by neurotrophins, whereby new GCs remain immature until becoming rapidly recruited to the network by activity.

摘要

随着年龄的增长,大脑会发生变化,从而损害认知能力和电路的可塑性,包括产生成人海马神经元的明显减少。目前尚不清楚这些新神经元的发育和整合是否也受到年龄的影响。在这里,我们表明,衰老小鼠中的新生颗粒细胞 (GCs) 数量稀少,发育缓慢,但它们具有显著的结构可塑性潜力。在中年小鼠中,用逆转录病毒标记的 3 周龄 GCs 体积小、发育不全且与网络断开连接。通过自愿运动或环境丰富可以加速神经元的发育和整合。通过敲低内源性神经营养因子受体负调节剂 Lrig1 也观察到类似的效果。一致地,通过 Lrig1 过表达阻断神经营养因子信号会消除运动的积极作用。这些结果表明,神经递质介导了衰老大脑中无与伦比的可塑性,新的 GCs 保持不成熟状态,直到通过活动被快速招募到网络中。

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