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本文引用的文献

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Cell adhesion molecule L1 modulates nerve-growth-factor-induced CGRP-IR fiber sprouting.细胞黏附分子L1调节神经生长因子诱导的降钙素基因相关肽免疫反应性纤维芽生。
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Injury reactive myelin/oligodendrocyte-derived axon growth inhibition in the adult mammalian central nervous system.
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Overcoming inhibitors in myelin to promote axonal regeneration.克服髓鞘中的抑制因子以促进轴突再生。
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Integrin activation and neurotrophin signaling cooperate to enhance neurite outgrowth in sensory neurons.整合素激活与神经营养因子信号传导协同作用,以增强感觉神经元的轴突生长。
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Chemorepulsion and cell adhesion molecules in patterning initial trajectories of sensory axons.化学排斥和细胞粘附分子在感觉轴突初始轨迹形成中的作用
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Myelin-, reactive glia-, and scar-derived CNS axon growth inhibitors: expression, receptor signaling, and correlation with axon regeneration.髓鞘、反应性胶质细胞和瘢痕衍生的中枢神经系统轴突生长抑制剂:表达、受体信号传导及其与轴突再生的相关性
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Semaphorin3A inhibits nerve growth factor-induced sprouting of nociceptive afferents in adult rat spinal cord.信号素3A抑制成年大鼠脊髓中神经生长因子诱导的伤害性传入神经纤维的发芽。
J Neurosci. 2004 Jan 28;24(4):819-27. doi: 10.1523/JNEUROSCI.1263-03.2004.
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Regeneration beyond the glial scar.超越胶质瘢痕的再生。
Nat Rev Neurosci. 2004 Feb;5(2):146-56. doi: 10.1038/nrn1326.
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Axonal regeneration through regions of chondroitin sulfate proteoglycan deposition after spinal cord injury: a balance of permissiveness and inhibition.脊髓损伤后轴突通过硫酸软骨素蛋白聚糖沉积区域的再生:许可与抑制的平衡
J Neurosci. 2003 Oct 15;23(28):9276-88. doi: 10.1523/JNEUROSCI.23-28-09276.2003.
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Toward full restoration of synaptic and terminal function of the dopaminergic system in Parkinson's disease by stem cells.通过干细胞实现帕金森病中多巴胺能系统突触和终末功能的完全恢复。
Ann Neurol. 2003;53 Suppl 3:S135-46; discussion S146-8. doi: 10.1002/ana.10482.

靶向成年中枢神经系统中沿预先形成的引导通路的神经元移植的轴突生长。

Targeting axon growth from neuronal transplants along preformed guidance pathways in the adult CNS.

作者信息

Ziemba Kristine S, Chaudhry Nagarathnamma, Rabchevsky Alexander G, Jin Ying, Smith George M

机构信息

Spinal Cord and Brain Injury Research Center, and Department of Physiology, University of Kentucky, Lexington, Kentucky 40536, USA.

出版信息

J Neurosci. 2008 Jan 9;28(2):340-8. doi: 10.1523/JNEUROSCI.3819-07.2008.

DOI:10.1523/JNEUROSCI.3819-07.2008
PMID:18184776
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6670506/
Abstract

To re-establish neuronal circuits lost after CNS injury, transplanted neurons must be able to extend axons toward their appropriate targets. Such growth is highly restricted within the adult CNS attributable to the expression of inhibitory molecules and general lack of guidance cues to direct axon growth. This environment typically induces random patterns of growth and aberrant innervation, if growth occurs at all. To target the growth of axons from neuronal transplants, we are using viral vectors to create guidance pathways before neuronal transplantation. In this study, we transplanted postnatal rat dorsal root ganglia neurons into the corpus callosum of adult rats. Replication-incompetent adenoviruses encoding growth or guidance factors were injected along the desired pathway 1 week before cell transplantation, allowing time for sufficient protein expression by host glial cells. With expression of nerve growth factor (NGF) and basic fibroblast growth factor, sensory axons were able to grow along the corpus callosum, across the midline, and toward an NGF-expressing target in either the contralateral striatum or cortex: a distance of 7-8 mm including a 90 degree turn from white matter into gray matter. Furthermore, expression of semaphorin 3A slightly dorsal and lateral to the turning point increased the number of axons turning into the striatal target. These results show that judicious expression of neuron-specific chemoattractant and chemorepellant molecules using viral vectors can support and target axon growth from neuronal transplants in the adult CNS.

摘要

为了重建中枢神经系统损伤后丧失的神经回路,移植的神经元必须能够将轴突延伸至其合适的靶标。在成年中枢神经系统内,这种生长受到高度限制,这归因于抑制性分子的表达以及普遍缺乏引导轴突生长的导向线索。如果轴突生长确实发生,这种环境通常会诱导随机的生长模式和异常的神经支配。为了引导神经元移植后的轴突生长,我们正在使用病毒载体在神经元移植前创建导向通路。在本研究中,我们将新生大鼠背根神经节神经元移植到成年大鼠的胼胝体中。在细胞移植前1周,沿着期望的通路注射编码生长或导向因子的无复制能力腺病毒,以便宿主胶质细胞有足够的时间进行蛋白质表达。随着神经生长因子(NGF)和碱性成纤维细胞生长因子的表达,感觉轴突能够沿着胼胝体生长,穿过中线,并朝着对侧纹状体或皮质中表达NGF的靶标生长:距离为7 - 8毫米,包括从白质到灰质的90度转弯。此外,在转折点稍背侧和外侧表达的信号素3A增加了转向纹状体靶标的轴突数量。这些结果表明,使用病毒载体明智地表达神经元特异性趋化因子和排斥因子分子,可以支持成年中枢神经系统中神经元移植后的轴突生长并引导其靶向生长。