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MOG诱导的实验性自身免疫性脑脊髓炎小鼠中枢及外周神经系统CD4^+ T及CD8^+ T调节性细胞变化 被引量:10

The change of periphery and centra CD4^+ CD25^+ Treg,CD8^+ CD28^- Treg in the MOG induced model of experimental autoimmune encephalomyelitis
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摘要 目的:观察实验性自身免疫性脑脊髓炎小鼠中枢及外周CD4^+CD25^+调节性T细胞(CD4^+CD25^+Treg),CD8^+CD28^-调节性T细胞(CD8^+CD28^-Treg)表达的变化情况,并探讨相关的细胞免疫学机制。方法:雌性C57BL/6小鼠随机分为未使用髓鞘少突胶质细胞糖蛋白35—55(MEVGWYR-SPFSRVVHLYRNGK)(MOG35-55)免疫的对照组和使用MOG35-55免疫诱导的EAE小鼠模型组,采用临床症状评分记录小鼠行为学变化、HE染色观察CNS炎症细胞浸润及病理改变,使用流式细胞术(FCM)检测小鼠中枢及外周CD8^+CD28^-Treg,CD4^+CD25^+Treg细胞表达水平。结果:MOG35-55诱导的EAE模型组动物出现典型的EAE临床行为学及病理学表现,FCM检测EAE模型组小鼠脾细胞CD4^+CD25^+Treg较对照组升高但无统计学差异,CD8^+CD28^-Treg表达水平明显低于对照组(P〈0.01),EAE模型组中枢有CD4^+CD25^+Treg,CD8^+CD28^-Treg淋巴细胞的浸润,且CD4^+CD25^+Treg,CD8^+CD28^-Treg在中枢的表达均高于外周,对照组中枢神经系统未检测到淋巴细胞浸润。结论:CD4^+CD25^+Treg,CD8^+CD28^-Treg均参与调控EAE的病理过程,CD4^+CD25^+Treg,CD8^+CD28^-Treg在EAE小鼠中枢及外周分布及变化的不同,提示其进人中枢神经系统(CNS)并参与调节中枢局部炎症。 AIM: To observe the change of periphery and centra CD4^+ CD25~ Treg, CD8^+ CD28^- Treg of MOG35-55 induced EAE disease in mouse, and to explore the potential mechanism of cellular immunity in the process of EAE. METHODS: MOG35-55 were used to establish EAE model on femina C57BL/6 mice. The behavioral changes and the histological scores were recorded. The changes of CD4^+ CD25^+ Treg, CD8^+ CD28^- Treg on periphery and centra lymphocyte in spleen , brain were analyzed by flow cytometry. RESULTS: MOG35-55-induced EAE group Showed the typical clinical behavior and pathological manifestations, CD4^+ CD25^+ Treg, CD8^+ CD28^- Treg lymphocytes were detected in the bran and spinal cord of EAE group mice, but they were not detected in the brain of control group. CD8^+ CD28^-Treg in the spleen of EAE group were lower than those in control group ( P 〈 0.01 ). CD4^+ CD25^+ Treg lymphocytes were slight higher than the control group. CONCLUSION: CD4^+ CD25^+ Treg, CD8^+ CD28^- Treg lymphocytes all play important roles in the pathogenesy of EAE. The distribution of CD4^+ CD25^+ Treg, CD8^+ CD28^- Treg in the CNS and peripheral of EAE is different, suggesting that their entry into the CNS and regulate of local inflammation.
出处 《细胞与分子免疫学杂志》 CAS CSCD 北大核心 2010年第8期746-749,共4页 Chinese Journal of Cellular and Molecular Immunology
基金 浙江省自然科学基金资助项目(Y207494)
关键词 CD4+ CD25+ TREG CD8+ CD28- TREG 实验性自身免疫性脑脊髓炎 多发性硬化 调节性T细胞 CD4^+ CD25^+ Treg CD8^+ CD28^- Treg experimental autoimmune encephalomyelitis multiple sclerosis regulatory T cell
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参考文献12

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