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作 者:侯国存[1] 陆江阳[1] 王宏伟[1] 刘茜[1] 田光[1] 杨毅[1] 李韶然[1]
机构地区:[1]解放军总医院第一附属医院(304医院)病理科,北京100048
出 处:《中国免疫学杂志》2009年第12期1063-1066,共4页Chinese Journal of Immunology
基 金:全军"十一五"医学科研项目基金资助项目(06MB307)
摘 要:目的:探讨CCR7在多器官功能障碍综合征(MODS)脾脏中的表达变化及其对树突状细胞(DC)迁移的影响。方法:用酵母多糖腹腔注射复制小鼠MODS模型,分为正常对照组和实验3-6小时组、24-48小时组、5-7天组及10-12天组。运用免疫组化方法检测CD11c和CD205标记阳性DC在各组小鼠脾脏中分布的变化,用流式细胞术检测CD86/CD11c和CCR7/CD11c标记阳性细胞在脾脏中含量的变化。结果:正常小鼠脾脏DC含量较少,主要分布在脾脏边缘区;在3-6小时组CCR7表达率较正常对照组显著增加,DC含量显著增加、活性增高,并向白髓T细胞区大量迁移;24-48小时组T细胞区中DC含量开始减少,而CCR7表达率升高达到峰值;5-7天组DC与CCR7含量接近正常对照组,边缘区和T细胞区均可见DC分布;10-12天组DC含量再次升高,但多呈不成熟状态,且以边缘区分布为主,CCR7表达率下降。结论:在MODS病程中脾脏DC的含量和分布变化与CCR7的表达率密切相关,CCR7可以作为评估脾脏DC迁移能力及功能活性的重要指标。Objective: To explore CCR7 expression in splenic dendritic cells and its role in migration and activity of splenic dendritic cells in multiple organ dysfunction syndrome (MODS) in mice. Methods: The MODS model of mice was reproduced by Zymosan injection into peritoneal cavity. The mice were randomly divided into groups of normal, 3-6 hours, 24-48 hours and 10-12 days post zymosan injection. CD1 l c and CD205 were analysed by immunohistochemistry; The expression of CD86 and CCR7 of DCs were studied by the flow cytometry analysis.Results:In normal mice,many DC were found at the margin between the red and white pulp.In the 3-6 h and 24-48 h greups, CD86 and CCR7 were strongly up-regulated in the DC, and they distributed in T cells areas. In the 10-12 d group, DC distributed at the margin by the immature form. Conclusion: The CCR7 expression level of DC has close correlations with the migration of DC, CCR7 can be used to evaluate the migration and functional activity of DC in MODS.
关 键 词:多器官功能障碍综合征 C族趋化因子受体-7 脾脏 树突状细胞
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