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脊髓损伤与神经元内在再生相关基因程序

Spinal cord injury and the neuron-intrinsic regeneration-associated gene program.

作者信息

Fagoe Nitish D, van Heest Jessica, Verhaagen Joost

机构信息

Laboratory for Neuroregeneration, Netherlands Institute for Neuroscience, an Institute of the Royal Academy of Arts and Sciences, Meibergdreef 47, 1105 BA, Amsterdam, The Netherlands,

出版信息

Neuromolecular Med. 2014 Dec;16(4):799-813. doi: 10.1007/s12017-014-8329-3. Epub 2014 Oct 1.

Abstract

Spinal cord injury (SCI) affects millions of people worldwide and causes a significant physical, emotional, social and economic burden. The main clinical hallmark of SCI is the permanent loss of motor, sensory and autonomic function below the level of injury. In general, neurons of the central nervous system (CNS) are incapable of regeneration, whereas injury to the peripheral nervous system is followed by axonal regeneration and usually results in some degree of functional recovery. The weak neuron-intrinsic regeneration-associated gene (RAG) response upon injury is an important reason for the failure of neurons in the CNS to regenerate an axon. This response consists of the expression of many RAGs, including regeneration-associated transcription factors (TFs). Regeneration-associated TFs are potential key regulators of the RAG program. The function of some regeneration-associated TFs has been studied in transgenic and knock-out mice and by adeno-associated viral vector-mediated overexpression in injured neurons. Here, we review these studies and propose that AAV-mediated gene delivery of combinations of regeneration-associated TFs is a potential strategy to activate the RAG program in injured CNS neurons and achieve long-distance axon regeneration.

摘要

脊髓损伤(SCI)影响着全球数百万人,并造成了巨大的身体、情感、社会和经济负担。SCI的主要临床特征是损伤平面以下运动、感觉和自主神经功能的永久性丧失。一般来说,中枢神经系统(CNS)的神经元无法再生,而外周神经系统损伤后会发生轴突再生,通常会导致一定程度的功能恢复。损伤后神经元内在再生相关基因(RAG)反应较弱是中枢神经系统神经元无法再生轴突的一个重要原因。这种反应包括许多RAG的表达,包括再生相关转录因子(TFs)。再生相关TFs是RAG程序的潜在关键调节因子。一些再生相关TFs的功能已在转基因和基因敲除小鼠中以及通过腺相关病毒载体介导在损伤神经元中过表达进行了研究。在此,我们综述这些研究,并提出通过腺相关病毒介导的再生相关TFs组合的基因递送是激活损伤中枢神经系统神经元中RAG程序并实现长距离轴突再生的潜在策略。

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