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流式细胞术揭示小鼠脊髓损伤后炎症反应的动态变化。

Dynamics of the inflammatory response after murine spinal cord injury revealed by flow cytometry.

作者信息

Stirling David P, Yong V Wee

机构信息

Hotchkiss Brain Institute and Department of Clinical Neurosciences, University of Calgary, Calgary, Alberta, Canada.

出版信息

J Neurosci Res. 2008 Jul;86(9):1944-58. doi: 10.1002/jnr.21659.

Abstract

Spinal cord injury (SCI) triggers a robust inflammatory response that contributes in part to the secondary degeneration of spared tissue. Here, we use flow cytometry to quantify the inflammatory response after SCI. Besides its objective evaluation, flow cytometry allows for levels of particular markers to be documented that further aid in the identification of cellular subsets. Analyses of blood from SCI mice for CD45 (common leukocyte antigen), CD11b (complement receptor-3), Gr-1 (neutrophil/monocyte marker), and CD3 (T-cell marker) revealed a marked increase in circulating neutrophils (CD45(high):Gr-1(high)) at 12 hr compared with controls. Monocyte density in blood increased at 24 hr, and in contrast, lymphocyte numbers were significantly decreased. Mirroring the early increase in neutrophils within the blood, flow analysis of the spinal cord lesion site revealed a significant (P < 0.01) and maintained increase in blood-derived leukocytes (CD45(high):CD11b(high)) from 12 to 96 hr compared with sham-injured and naive controls. Importantly, this technique clearly distinguishes blood-derived neutrophils (CD45:Gr-1(high):F4/80(negative)) and monocyte/macrophages (CD45(high)) from resident microglia (CD45(low)) and revealed that the majority of the blood-derived infiltrate were neutrophils. Our results highlight an assumed, but previously uncharacterized, marked and transient increase in leukocyte populations in blood early after SCI followed by the orchestrated invasion of neutrophils and monocytes into the injured cord. In contrast to mobilization of neutrophils, SCI induces lymphopenia that may contribute negatively to the overall outcome after spinal cord trauma.

摘要

脊髓损伤(SCI)会引发强烈的炎症反应,这在一定程度上导致了未受损组织的继发性退化。在此,我们使用流式细胞术来量化脊髓损伤后的炎症反应。除了客观评估外,流式细胞术还能记录特定标志物的水平,这有助于进一步识别细胞亚群。对脊髓损伤小鼠血液中的CD45(共同白细胞抗原)、CD11b(补体受体-3)、Gr-1(中性粒细胞/单核细胞标志物)和CD3(T细胞标志物)进行分析,结果显示,与对照组相比,损伤后12小时循环中性粒细胞(CD45(高):Gr-1(高))显著增加。血液中的单核细胞密度在24小时时增加,相反,淋巴细胞数量显著减少。与血液中中性粒细胞的早期增加相一致,对脊髓损伤部位的流式分析显示,与假手术组和未受伤对照组相比,损伤后12至96小时血液来源的白细胞(CD45(高):CD11b(高))显著(P < 0.01)且持续增加。重要的是,该技术能够清楚地区分血液来源的中性粒细胞(CD45:Gr-1(高):F4/80(阴性))和单核细胞/巨噬细胞(CD45(高))与驻留小胶质细胞(CD45(低)),并显示血液来源的浸润细胞大多数是中性粒细胞。我们的研究结果突出了脊髓损伤后早期血液中白细胞群体假定但此前未被描述的显著且短暂的增加,随后是中性粒细胞和单核细胞有序侵入受损脊髓。与中性粒细胞的动员相反,脊髓损伤会导致淋巴细胞减少,这可能对脊髓创伤后的总体结果产生负面影响。

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