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本文引用的文献

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Restoring voluntary control of locomotion after paralyzing spinal cord injury.恢复瘫痪性脊髓损伤后的自主运动控制。
Science. 2012 Jun 1;336(6085):1182-5. doi: 10.1126/science.1217416.
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Repetitive spinal electromagnetic stimulation opens a window of synaptic plasticity in damaged spinal cord: role of NMDA receptors.重复的脊髓电磁刺激在受损脊髓中打开了突触可塑性的窗口:NMDA 受体的作用。
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Differential effects of brain-derived neurotrophic factor and neurotrophin-3 on hindlimb function in paraplegic rats.脑源性神经营养因子和神经营养因子-3 对截瘫大鼠后肢功能的不同影响。
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Chondroitinase ABC combined with neurotrophin NT-3 secretion and NR2D expression promotes axonal plasticity and functional recovery in rats with lateral hemisection of the spinal cord.软骨素酶 ABC 联合神经营养因子 NT-3 的分泌和 NR2D 表达促进大鼠脊髓侧半横断后轴突可塑性和功能恢复。
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Combined delivery of Nogo-A antibody, neurotrophin-3 and the NMDA-NR2d subunit establishes a functional 'detour' in the hemisected spinal cord.Nogo-A 抗体、神经营养因子-3 和 NMDA-NR2d 亚基联合递呈在脊髓半切损伤中建立功能性“旁路”。
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Alterations in chondroitin sulfate proteoglycan expression occur both at and far from the site of spinal contusion injury.软骨素硫酸盐蛋白聚糖的表达改变既发生在脊髓挫伤损伤部位,也发生在远离损伤部位的地方。
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Chondroitin sulphate proteoglycans: key modulators of spinal cord and brain plasticity.硫酸软骨素蛋白聚糖:脊髓和大脑可塑性的关键调节物。
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10
Intermittent fasting improves functional recovery after rat thoracic contusion spinal cord injury.间歇性禁食可改善大鼠胸段挫伤性脊髓损伤后的功能恢复。
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抑制分子 NG2 的中和作用可改善成年大鼠脊髓损伤后的突触传递、逆行运输和运动功能。

Neutralization of inhibitory molecule NG2 improves synaptic transmission, retrograde transport, and locomotor function after spinal cord injury in adult rats.

机构信息

Northport Veterans Affairs Medical Center, Northport, New York 11768, USA.

出版信息

J Neurosci. 2013 Feb 27;33(9):4032-43. doi: 10.1523/JNEUROSCI.4702-12.2013.

DOI:10.1523/JNEUROSCI.4702-12.2013
PMID:23447612
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6619302/
Abstract

NG2 belongs to the family of chondroitin sulfate proteoglycans that are upregulated after spinal cord injury (SCI) and are major inhibitory factors restricting the growth of fibers after SCI. Neutralization of NG2's inhibitory effect on axon growth by anti-NG2 monoclonal antibodies (NG2-Ab) has been reported. In addition, recent studies show that exogenous NG2 induces a block of axonal conduction. In this study, we demonstrate that acute intraspinal injections of NG2-Ab prevented an acute block of conduction by NG2. Chronic intrathecal infusion of NG2-Ab improved the following deficits induced by chronic midthoracic lateral hemisection (HX) injury: (1) synaptic transmission to lumbar motoneurons, (2) retrograde transport of fluororuby anatomical tracer from L5 to L1, and (3) locomotor function assessed by automated CatWalk gait analysis. We collected data in an attempt to understand the cellular and molecular mechanisms underlying the NG2-Ab-induced improvement of synaptic transmission in HX-injured spinal cord. These data showed the following: (1) that chronic NG2-Ab infusion improved conduction and axonal excitability in chronically HX-injured rats, (2) that antibody treatment increased the density of serotonergic axons with ventral regions of spinal segments L1-L5, (3) and that NG2-positive processes contact nodes of Ranvier within the nodal gap at the location of nodal Na(+) channels, which are known to be critical for propagation of action potentials along axons. Together, these results demonstrate that treatment with NG2-Ab partially improves both synaptic and anatomical plasticity in damaged spinal cord and promotes functional recovery after HX SCI. Neutralizing antibodies against NG2 may be an excellent way to promote axonal conduction after SCI.

摘要

NG2 属于软骨素硫酸盐蛋白聚糖家族,在脊髓损伤(SCI)后上调,是限制 SCI 后纤维生长的主要抑制因子。已有报道称,抗 NG2 单克隆抗体(NG2-Ab)可中和 NG2 对轴突生长的抑制作用。此外,最近的研究表明,外源性 NG2 可诱导轴突传导阻滞。在本研究中,我们证明急性脊髓内注射 NG2-Ab 可防止 NG2 引起的急性传导阻滞。慢性鞘内输注 NG2-Ab 改善了慢性中胸侧半横断(HX)损伤引起的以下缺陷:(1)对腰运动神经元的突触传递,(2)荧光素 retrograde 从 L5 到 L1 的解剖示踪剂运输,以及(3)通过自动 CatWalk 步态分析评估的运动功能。我们收集了数据,试图了解 NG2-Ab 诱导的 HX 损伤脊髓中突触传递改善的细胞和分子机制。这些数据显示:(1)慢性 NG2-Ab 输注可改善慢性 HX 损伤大鼠的传导和轴突兴奋性,(2)抗体治疗增加了 L1-L5 脊髓节段腹侧区域的 5-羟色胺能轴突密度,(3)NG2 阳性过程接触节间 Na+通道所在位置的Ranvier 结的节点间隙中的节点 Na+通道,已知这些通道对于动作电位沿轴突传播至关重要。综上所述,这些结果表明,NG2-Ab 治疗可部分改善损伤脊髓中的突触和解剖可塑性,并促进 HX SCI 后的功能恢复。针对 NG2 的中和抗体可能是促进 SCI 后轴突传导的一种极好方法。