针对生殖道沙眼衣原体感染的保护性CD4 + T细胞介导免疫的差异性CD28和诱导性共刺激分子信号需求
Differential CD28 and inducible costimulatory molecule signaling requirements for protective CD4+ T-cell-mediated immunity against genital tract Chlamydia trachomatis infection.
作者信息
Marks Ellen, Verolin Martina, Stensson Anneli, Lycke Nils
机构信息
Department of Microbiology and Immunology, Mucosal Immunobiology and Vaccine Research Center, Institute of Biomedicine, Gothenburg University, Box 435, 40530 Gothenburg, Sweden.
出版信息
Infect Immun. 2007 Sep;75(9):4638-47. doi: 10.1128/IAI.00465-07. Epub 2007 Jul 16.
Th1 cells and gamma interferon (IFN-gamma) production play critical roles in protective immunity against genital tract infections by Chlamydia trachomatis. Here we show that inducible costimulatory molecule (ICOS)(-/-) mice develop greatly augmented host resistance against chlamydial infection. Protection following a primary infection was characterized by strong Th1 immunity with enhanced CD4(+) T-cell-mediated IFN-gamma production in the genital tract and high expression of T-bet in the draining para-aortic lymph node. This Th1 dominance was associated with low expression of interleukin 10 (IL-10) mRNA in the uteruses of protected ICOS(-/-) mice. By contrast, CD28(-/-) mice were severely impaired in their adaptive immune response, demonstrating a lack of CD4(+) T cells and IFN-gamma in the genital tract, with a substantial delay in bacterial elimination compared to that seen in wild-type (WT) mice. Upon reinfection, WT mice exhibited a transient local infection with evidence of regulatory T-cell (Treg)/Foxp3 mRNA and a more balanced Th1 and Th2 response in the genital tract than ICOS(-/-) mice, whereas 90% of the latter mice developed sterile immunity, poor expression of local Treg/Foxp3 mRNA, and macroscopic signs of enhanced local immunopathology. Therefore, different requirements for CD28 signaling and ICOS signaling clearly apply to host protection against a genital tract infection by C. trachomatis. Whereas, CD28 signaling is critical, ICOS appears to be dispensable and can have a dampening effect on Th1 development by driving Th2 immunity and anti-inflammation through IL-10 production and promotion of the Foxp3(+) Treg populations in the genital tract. Both the CD28-deficient and the ICOS-deficient mice demonstrated poor specific antibody production, supporting the fact that antibodies are not needed for protection against genital tract chlamydial infections.
辅助性T细胞1(Th1细胞)和γ干扰素(IFN-γ)的产生在针对沙眼衣原体生殖道感染的保护性免疫中发挥关键作用。在此我们表明,诱导性共刺激分子(ICOS)基因敲除小鼠对衣原体感染的宿主抵抗力大幅增强。初次感染后的保护作用表现为强大的Th1免疫,其特征是生殖道中CD4⁺ T细胞介导的IFN-γ产生增强,以及引流的主动脉旁淋巴结中T-bet的高表达。这种Th1优势与受保护的ICOS基因敲除小鼠子宫中白细胞介素10(IL-10)mRNA的低表达相关。相比之下,CD28基因敲除小鼠的适应性免疫反应严重受损,表现为生殖道中缺乏CD4⁺ T细胞和IFN-γ,与野生型(WT)小鼠相比,细菌清除明显延迟。再次感染时,WT小鼠表现为短暂的局部感染,有调节性T细胞(Treg)/Foxp3 mRNA的证据,且生殖道中Th1和Th2反应比ICOS基因敲除小鼠更平衡,而后者中90%的小鼠产生了无菌免疫,局部Treg/Foxp3 mRNA表达不佳,并有局部免疫病理学增强的宏观迹象。因此,CD28信号传导和ICOS信号传导的不同需求显然适用于宿主针对沙眼衣原体生殖道感染的保护。虽然CD28信号传导至关重要,但ICOS似乎是可有可无的,并且通过驱动Th2免疫和通过IL-10产生及促进生殖道中Foxp3⁺ Treg群体来促进抗炎作用,可能对Th1发育有抑制作用。CD28缺陷和ICOS缺陷小鼠均表现出特异性抗体产生不佳,支持了抗体对预防生殖道衣原体感染并非必需这一事实。
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