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Recapitulate development to promote axonal regeneration: good or bad approach?

机译:概述促进轴突再生的发展:好方法还是坏方法?

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摘要

In the past decade there has been an explosion in our understanding, at the molecular level, of why axons in the adult, mammalian central nervous system (CNS) do not spontaneously regenerate while their younger counterparts do. Now a number of inhibitors of axonal regeneration have been described, some of the receptors they interact with to transduce the inhibitory signal are known, as are some of the steps in the signal transduction pathway that is responsible for inhibition. In addition, developmental changes in the environment and in the neurons themselves are also now better understood. This knowledge in turn reveals novel, putative sites for drug development and therapeutic intervention after injury to the brain and spinal cord. The challenge now is to determine which of these putative treatments are the most effective and if they would be better applied in combination rather than alone. In this review I will summarize what we have learnt about these molecules and how they signal. Importantly, I will also describe approches that have been shown to block inhibitors and encourage regeneration in vivo. I will also speculate on what the differences are between the neonatal and adult CNS that allow the former to regenerate and the latter not to.
机译:在过去的十年中,在分子水平上,关于为什么成年哺乳动物中枢神经系统(CNS)中的轴突不能自发再生,而年轻的同行者却会自发再生的理解已经激增。现在已经描述了许多轴突再生抑制剂,与它们相互作用以转导抑制信号的一些受体是已知的,信号转导途径中负责抑制的一些步骤也是已知的。此外,现在也更好地理解了环境和神经元本身的发育变化。这些知识反过来揭示了在大脑和脊髓受伤后进行药物开发和治疗干预的新的推测位点。现在的挑战是确定这些推定的治疗方法中哪一种最有效,以及它们是否可以更好地组合使用而不是单独使用。在这篇综述中,我将总结我们对这些分子以及它们如何发出信号的了解。重要的是,我还将描述已证明能阻止抑制剂并促进体内再生的方法。我还将推测新生儿和成人中枢神经系统之间的区别是,前者可以再生而后者则不能再生。

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