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成年大鼠中嗅鞘细胞或外周轴突切断对背柱轴突再生反应的影响

Modification of the regenerative response of dorsal column axons by olfactory ensheathing cells or peripheral axotomy in adult rat.

作者信息

Andrews Melissa R, Stelzner Dennis J

机构信息

Department of Cell and Developmental Biology, State University of New York Upstate Medical University, Syracuse, NY 13210, USA.

出版信息

Exp Neurol. 2004 Dec;190(2):311-27. doi: 10.1016/j.expneurol.2004.08.011.

DOI:10.1016/j.expneurol.2004.08.011
PMID:15530871
Abstract

The regeneration of sciatic-dorsal column (DC) axons following DC crush injury and treatment with olfactory ensheathing cells (OECs) and/or sciatic axotomy ("conditioning lesion") was evaluated. Sciatic-DC axons were examined with a transganglionic tracer, cholera toxin conjugated to horseradish peroxidase, and evaluated at chronic time points, 2-26 weeks post-lesion. With DC injury alone (n = 7), sciatic-DC axons were localized to the caudal border of the lesion terminating in reactive end bulbs with no indication of growth into the lesion. In contrast, treatment with either a heterogeneous population of OECs (equal numbers of p75- and fibronectin-positive OECs) (n = 9) or an enriched population of OECs (75% p75-positive OECs) (n = 6) injected either directly into the lesion or 1-mm rostral and caudal to the injury, stimulated DC axon growth into the lesion. A similar regenerative response was observed with a conditioning lesion either concurrent to (n = 4) or 1 week before (n = 4) the DC injury. In either of the latter two paradigms, some DC axons grew across the injury, but no axons grew into the rostral intact spinal cord. Upon combining OEC treatment with the conditioning lesion (n = 21), the result was additive, increasing DC axon growth beyond the rostral border of the lesion in best cases. Additional factors that may limit DC regeneration were tested including formation of the glial scar (immunoreactivity to glial fibrillary acidic protein in astrocytes and to chondroitin sulfate proteoglycans), which remained similar between treated and untreated groups.

摘要

评估了坐骨神经-背柱(DC)轴突在DC挤压伤后,以及用嗅鞘细胞(OECs)和/或坐骨神经轴突切断术(“预处理损伤”)治疗后的再生情况。使用与辣根过氧化物酶偶联的霍乱毒素这种跨神经节示踪剂来检测坐骨神经-DC轴突,并在损伤后2至26周的慢性时间点进行评估。仅进行DC损伤时(n = 7),坐骨神经-DC轴突定位于损伤的尾侧边界,终止于反应性终球,没有向损伤部位生长的迹象。相比之下,将异质性OEC群体(p75阳性和纤连蛋白阳性OEC数量相等)(n = 9)或富集的OEC群体(75% p75阳性OEC)(n = 6)直接注射到损伤部位或损伤部位头侧和尾侧1毫米处,可刺激DC轴突向损伤部位生长。在DC损伤同时(n = 4)或之前1周(n = 4)进行预处理损伤时,观察到了类似的再生反应。在后两种模式中的任何一种情况下,一些DC轴突跨越损伤部位生长,但没有轴突生长到头侧完整的脊髓中。将OEC治疗与预处理损伤相结合(n = 21)时,结果是相加的,在最佳情况下可增加DC轴突向损伤部位头侧边界以外的生长。还测试了可能限制DC再生的其他因素,包括胶质瘢痕的形成(星形胶质细胞中胶质纤维酸性蛋白和硫酸软骨素蛋白聚糖的免疫反应性),治疗组和未治疗组之间保持相似。

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Front Cell Neurosci. 2021 Nov 17;15:781489. doi: 10.3389/fncel.2021.781489. eCollection 2021.
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The Extracellular Environment of the CNS: Influence on Plasticity, Sprouting, and Axonal Regeneration after Spinal Cord Injury.中枢神经系统的细胞外环境:对脊髓损伤后可塑性、发芽和轴突再生的影响。
Neural Plast. 2018 Apr 18;2018:2952386. doi: 10.1155/2018/2952386. eCollection 2018.
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The Dorsal Column Lesion Model of Spinal Cord Injury and Its Use in Deciphering the Neuron-Intrinsic Injury Response.
脊髓损伤的背柱损伤模型及其在破译神经元内在损伤反应中的应用。
Dev Neurobiol. 2018 Oct;78(10):926-951. doi: 10.1002/dneu.22601. Epub 2018 May 11.
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Biomaterial Approaches to Enhancing Neurorestoration after Spinal Cord Injury: Strategies for Overcoming Inherent Biological Obstacles.脊髓损伤后促进神经修复的生物材料方法:克服内在生物学障碍的策略
Biomed Res Int. 2015;2015:752572. doi: 10.1155/2015/752572. Epub 2015 Sep 27.
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GDNF selectively promotes regeneration of injury-primed sensory neurons in the lesioned spinal cord.胶质细胞源性神经营养因子选择性地促进损伤引发的脊髓感觉神经元在受损脊髓中的再生。
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