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成年中枢神经系统损伤后的可塑性:重现发育状态值得促进吗?

Plasticity following injury to the adult central nervous system: is recapitulation of a developmental state worth promoting?

作者信息

Emery Dana L, Royo Nicolas C, Fischer Itzhak, Saatman Kathryn E, McIntosh Tracy K

机构信息

Head Injury Center, Department of Neurosurgery, University of Pennsylvania, USA.

出版信息

J Neurotrauma. 2003 Dec;20(12):1271-92. doi: 10.1089/089771503322686085.

Abstract

The adult central nervous system (CNS) appears to initiate a transient increase in plasticity following injury, including increases in growth-related proteins and generation of new cells. Recent evidence is reviewed that the injured adult CNS exhibits events and patterns of gene expression that are also observed during development and during regeneration following damage to the mature peripheral nervous system (PNS). The growth of neurons during development or regeneration is correlated, in part, with a coordinated expression of growth-related proteins, such as growth-associated-protein-43 (GAP-43), microtubule-associated-protein-1B (MAP1B), and polysialylated-neural-cell-adhesion-molecule (PSA-NCAM). For each of these proteins, evidence is discussed regarding its specific role in neuronal development, signals that modify its expression, and reappearance following injury. The rate of adult hippocampal neurogenesis is also affected by numerous endogenous and exogenous factors including injury. The continuing study of developmental neurobiology will likely provide further gene and protein targets for increasing plasticity and regeneration in the mature adult CNS.

摘要

成体中枢神经系统(CNS)在损伤后似乎会引发可塑性的短暂增加,包括与生长相关的蛋白质增加和新细胞的生成。本文综述了近期的证据,即受损的成体CNS表现出在发育过程以及成熟外周神经系统(PNS)损伤后的再生过程中也能观察到的基因表达事件和模式。神经元在发育或再生过程中的生长,部分与生长相关蛋白质的协调表达有关,如生长相关蛋白-43(GAP-43)、微管相关蛋白-1B(MAP1B)和多唾液酸神经细胞黏附分子(PSA-NCAM)。针对这些蛋白质中的每一种,本文都讨论了其在神经元发育中的具体作用、调节其表达的信号以及损伤后的重新出现。成体海马神经发生的速率也受到包括损伤在内的多种内源性和外源性因素的影响。对发育神经生物学的持续研究可能会为增加成熟成体CNS的可塑性和再生提供更多的基因和蛋白质靶点。

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