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MyD88在鼠衣原体生殖道感染过程中的作用 被引量:7

The Roles of MyD88 in the Development of Protective Immunity and Pathology During Chlamydial Urogenital Infection in Mice
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摘要 用1×104IFUs的MoPn经生殖道感染WT、MyD88 KO小鼠,每组一半小鼠于感染后54d,再次感染相同剂量的MoPn。每隔3-4d取生殖道分泌物,测定其中衣原体包涵体的数量。初次感染后80d,处死小鼠,眼眶取血,分离血清,用间接免疫荧光法测其中抗体类型及效价;同时分离生殖道,肉眼观察其输卵管、子宫角水肿程度,并做病理切片观察其炎症反应;分离小鼠脾细胞,体外用衣原体EB刺激,测定产生的IL-4、IL-5、IL-17和IFN-γ等细胞因子水平。MyD88 KO小鼠阴道带菌时间与WT组相当,但上生殖道病理反应,尤其是输卵管水肿程度明显比WT组严重。脾细胞细胞因子水平显示,MyD88 KO鼠IFN-γ和IL-17的产生量明显比WT组低,而IL-4和IL-5水平明显高于WT组。血清中各亚类抗体效价无明显区别,但MyD88 KO鼠血清IgG2a/IgG1比值<1,且明显低于WT组。研究结果说明MyD88与抗衣原体免疫无关,但与衣原体引起的炎症损伤密切相关。 C57BL/6J WT and mice deficient in MyD88(MyD88 KO) were inoculated intravaginally with 1 × 104 IFUs of live C.muridarum organisms.Half mice of each group were reinfected on day 54 after primary infection.Vaginal swabs were taken every 3 or 4 days to monitor live organism shedding.On day 80 after the primary infection,mice were sacrificed,and the vaginal tract was isolated for pathology.The spleen cells were collected and IL-4,IL-5,IL-17 and IFN-γ were detected by ELISA in the spleen cells culture supernatant after restimulated by MoPn EB.The titers of different Ab isotypes were measured in mice serum by Indirect Immunofluorescence Assay.The Chlamydia shedding time of MyD88 KO mice was similar to WT.Not only the gross appearance of the isolated genital tracts,but also the dilation and inflammation scores under microscope showed that the genital tract pathology from the MyD88-deficient mice was much more severe than WT after primary infection.The results of Th2(IL-4 IL-5),Th1(IFN-γ) and Th17(IL-17) cytokines from the in vitro restimulated splenocyte culture supernatant showed that MyD88 deficient mice produced significantly lower levels of IFN-γ and IL-17 but much higher levels of IL-4 and IL-5 than WT mice either after the primary infection or reinfection with Chlamydia.There were no significant differences in Ab isotype levels between the two tested groups.However,the ratio of MoPn specific serum IgG2a/IgG1 in MyD88-deficient mice was less than 1 and significantly lower than that in WT mice.MyD88 is dispensable for protective immunity but required for inflammatory pathologies.
作者 陈丽丽 吴移谋 周洲 雷磊 蔡恒玲 钟光明
机构地区 南华大学病原生物学研究所 Department of Microbiology and Immunology
出处 《微生物学通报》 CAS CSCD 北大核心 2010年第6期937-942,共6页 Microbiology China
基金 湖南省科技厅基金项目(No2009FJ3207) US National Institute of Health基金项目(No1R01AI47997-01)
关键词 鼠衣原体(MoPn) MYD88 泌尿生殖道感染 病理 Chlamydia muridarum MyD88 Urogenital tract infection Pathology
分类号 R759 [医药卫生—皮肤病学与性病学]
  • 相关文献

参考文献13

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二级参考文献69

  • 1李跃华,哈团柱,陈琪,李传富.MyD88依赖性核因子-κB信号途径在心肌肥大发生过程中的调控作用[J].中华医学杂志,2005,85(4):267-272. 被引量:19
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共引文献40

同被引文献94

  • 1李跃华,哈团柱,陈琪,李传富.MyD88依赖性核因子-κB信号途径在心肌肥大发生过程中的调控作用[J].中华医学杂志,2005,85(4):267-272. 被引量:19
  • 2王乐丹,张丽芳.沙眼衣原体主要外膜蛋白抗原表位的研究进展[J].国外医学(预防.诊断.治疗用生物制品分册),2005,28(5):196-199. 被引量:1
  • 3陈丽丽,吴移谋,雷达,吴志周,黄澍杰.泌尿生殖道沙眼衣原体omp1基因多态性研究[J].微生物学报,2006,46(2):214-218. 被引量:8
  • 4Barteneva N, Theodor I, Peterson EM, et al. Role of neutrophils in controlling early stages of a Chlamydia trachomatis infection, lnfect lmmun, 1996, 64(11): 4830-4833.
  • 5Ito JI, Lyons JM. Role of gamma interferon in controlling murine chlamydial genital tract infection. Infect Immun, 1999, 67(10): 5518-5521.
  • 6Kawai T, Adachi O, Ogawa T, et al. Unresponsiveness of MyD88 dificient mice to endotoxin. Immunity, 1999, 11(1): 115-122.
  • 7Arbour NC, Lorenz E, Schutte BC, et al. TLR4 mutations are associated with endotoxin hyporesponsiveness in humans. Nat Genet, 2000, 25(2): 187-191.
  • 8Brunham RC, Rey-Ladino J. Immunology of Chlamydia infection: implications for a Chlamydia trachomatis vaccine[J]. Nature Reviews Immunology, 2005, 5(2): 149-161.
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微生物学通报
2010年 第6期

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