首页> 外文期刊>Molecular Neurobiology >Maintaining the neuronal phenotype after injury in the adult CNS. Neurotrophic factors, axonal growth substrates, and gene therapy.
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Maintaining the neuronal phenotype after injury in the adult CNS. Neurotrophic factors, axonal growth substrates, and gene therapy.

机译:在成人中枢神经系统损伤后维持神经元表型。神经营养因子,轴突生长底物和基因治疗。

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Multiple genetic and epigenetic events determine neuronal phenotype during nervous system development. After the mature mammalian neuronal phenotype has been determined it is usually static for the remainder of life, unless an injury or degenerative event occurs. Injured neurons may suffer one of three potential fates: death, persistent atrophy, or recovery. The ability of an injured adult neuron to recover from injury in adulthood may be determined by events that also influence neuronal phenotype during development, including expression of growth-related genes and responsiveness to survival and growth signals in the environment. The latter signals include neurotrophic factors and substrate molecules that promote neurite growth. Several adult CNS regions exhibit neurotrophic-factor responsiveness, including the basal forebrain, entorhinal cortex, hippocampus, thalamus, brainstem, and spinal cord. The specificity of neurotrophic-factor responsiveness in these regions parallels patterns observed during development. In addition, neurons of several CNS regions extend neurites after injury when presented with growth-promoting substrates. When both neurotrophic factors and growth-promoting substrates are provided to adult rats that have undergone bilateral fimbria-fornix lesions, then partial morphological and behavioral recovery can be induced. Gene therapy is one useful tool for providing these substances. Thus, the mature CNS remains robustly responsive to signals that shape nervous system development, and is highly plastic when stimulated by appropriate cues.
机译:在神经系统发育过程中,多种遗传和表观遗传事件决定了神经元表型。确定成熟的哺乳动物神经元表型后,在其余生命中通常是静态的,除非发生损伤或变性事件。受伤的神经元可能遭受三种潜在命运之一:死亡,持续萎缩或恢复。受伤的成年神经元恢复成年后受伤的能力可能取决于在发育过程中也会影响神经元表型的事件,包括生长相关基因的表达以及对环境中生存和生长信号的响应能力。后者的信号包括神经营养因子和促进神经突生长的底物分子。几个成年的中枢神经系统区域表现出神经营养因子反应性,包括基底前脑,内嗅皮层,海马,丘脑,脑干和脊髓。在这些区域中神经营养因子反应的特异性与发育过程中观察到的模式相似。另外,当存在促进生长的底物时,多个CNS区域的神经元在损伤后延伸神经突。当神经营养因子和促进生长的底物同时提供给经历了双侧纤毛-穹lesions损伤的成年大鼠时,则可以诱导部分形态和行为恢复。基因疗法是提供这些物质的一种有用工具。因此,成熟的中枢神经系统对形成神经系统发育的信号仍然具有强烈的响应能力,并且在受到适当提示的刺激下具有很高的可塑性。

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