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周围神经损伤后大鼠脊髓细胞增殖的特征及其与神经性疼痛的关系。

Characterization of cell proliferation in rat spinal cord following peripheral nerve injury and the relationship with neuropathic pain.

作者信息

Echeverry Stefania, Shi Xiang Qun, Zhang Ji

机构信息

Unité de Neurobiologie Cellulaire, Centre de Recherche Université Laval Robert-Giffard, Université Laval, 2601, Chemin de la Canardière, Québec, Canada.

出版信息

Pain. 2008 Mar;135(1-2):37-47. doi: 10.1016/j.pain.2007.05.002. Epub 2007 Jun 8.

Abstract

Glial activation is a typical response of the central nervous system to nerve injury. In the current investigation, we characterized the temporal and spatial pattern of glial proliferation, one of the most conspicuous features of glial activation, in relation to nerve injury-induced neuropathic pain. Using bromodeoxyuridine (BrdU) as a mitotic marker, we analyzed cell proliferation in the spinal cord, identified the phenotype of dividing cells, traced their fate, and correlated these phenomena with behavioural assays of the neuropathic pain syndrome. Our results demonstrated that peripheral nerve injury induced an early and transient cell proliferation, on the spinal cord ipsilateral to the nerve lesion which peaked at day 3 post-surgery. The majority of the proliferating cells were Iba-1(+) microglia, together with some NG2(+) oligodendrocyte progenitors, and GFAP(+) astrocytes. These newly generated cells continued to divide over time with the response peaking at day 14 post-injury. Microglia were always the predominant phenotype which made up over 60% of activated microglia derived from this newly generated cell population. There was a close temporal correlation between microglial proliferation in the spinal cord dorsal horn and the abnormal pain responses, suggesting a contribution of the new microglia to the genesis of the neuropathic pain symptoms.

摘要

胶质细胞激活是中枢神经系统对神经损伤的典型反应。在本研究中,我们描述了胶质细胞增殖的时空模式,胶质细胞增殖是胶质细胞激活最显著的特征之一,与神经损伤诱导的神经性疼痛相关。我们使用溴脱氧尿苷(BrdU)作为有丝分裂标记物,分析脊髓中的细胞增殖,确定分裂细胞的表型,追踪它们的命运,并将这些现象与神经性疼痛综合征的行为学检测结果相关联。我们的结果表明,外周神经损伤在神经损伤同侧的脊髓中诱导了早期短暂的细胞增殖,在术后第3天达到峰值。大多数增殖细胞是Iba-1(+)小胶质细胞,还有一些NG2(+)少突胶质前体细胞和GFAP(+)星形胶质细胞。这些新生成的细胞随着时间的推移持续分裂,在损伤后第14天反应达到峰值。小胶质细胞始终是主要表型,占源自这个新生成细胞群体的活化小胶质细胞的60%以上。脊髓背角小胶质细胞增殖与异常疼痛反应之间存在密切的时间相关性,表明新生成的小胶质细胞对神经性疼痛症状的发生有贡献。

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