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念珠菌病小鼠早期T细胞无反应性及IL-2的逆转作用:对辅助性T细胞发育的影响

Early T cell unresponsiveness in mice with candidiasis and reversal by IL-2: effect on T helper cell development.

作者信息

Spaccapelo R, Del Sero G, Mosci P, Bistoni F, Romani L

机构信息

Department of Experimental Medicine and Biochemical Sciences, University of Perugia, Italy.

出版信息

J Immunol. 1997 Mar 1;158(5):2294-302.

PMID:9036977
Abstract

To investigate the role and effect of IL-2 in the genesis of Th1 and Th2 responses to Candida albicans in vivo, we assessed the levels of IL-2 production and the Ag-specific proliferative response in mice with healing or nonhealing infection and the effects of IL-2 neutralization or administration on the course and outcome of infection and on the type of CD4+ Th immunity elicited. High levels of IL-2 production and Ag-specific proliferation in vitro correlated with disease progression in susceptible mice. In contrast, resolution of infection in resistant mice was accompanied by the induction of Ag-specific hyporesponsiveness and impaired IL-2 production. Progression of infection did not occur in susceptible mice treated with anti-IL-2 or anti-IL-2R mAbs; conversely, disease resolution was prevented in resistant mice treated with IL-2. CD4+ Th1 cell responses were present in BALB/c mice rendered resistant by IL-2 neutralization and CD4+ Th2 responses in mice rendered susceptible by IL-2 treatment. The presence of IL-2 restored Ag-specific responsiveness in vitro and correlated in vivo with the expansion of CD4+ MEL-149(low) cells capable of producing IL-2 and IL-4 both in vitro and in vivo as observed in adult thymectomized mice. These results indicate that production of IL-2 early in infection correlates with the induction of IL-4-producing CD4+ Th2 cells, while a transient loss of T cell responsiveness, such as IL-2 production, appears to be required for CD4+ Th1 occurrence in mice with candidiasis.

摘要

为了研究白细胞介素-2(IL-2)在体内对白色念珠菌的Th1和Th2反应发生过程中的作用及影响,我们评估了感染愈合或未愈合小鼠体内IL-2的产生水平和抗原特异性增殖反应,以及IL-2中和或给予对感染进程和结果以及所引发的CD4+ Th免疫类型的影响。体外高水平的IL-2产生和抗原特异性增殖与易感小鼠的疾病进展相关。相反,抗性小鼠感染的消退伴随着抗原特异性低反应性的诱导和IL-2产生受损。用抗IL-2或抗IL-2R单克隆抗体治疗的易感小鼠未出现感染进展;相反,用IL-2治疗的抗性小鼠的疾病消退受到阻碍。在通过IL-2中和而产生抗性的BALB/c小鼠中存在CD4+ Th1细胞反应,在通过IL-2治疗而变得易感的小鼠中存在CD4+ Th2反应。IL-2的存在恢复了体外抗原特异性反应性,并且在体内与能够在体外和体内产生IL-2和IL-4的CD4+ MEL-149(low)细胞的扩增相关,这在成年胸腺切除小鼠中也有观察到。这些结果表明,感染早期IL-2的产生与产生IL-4的CD4+ Th2细胞的诱导相关,而对于念珠菌病小鼠中CD4+ Th1的出现,似乎需要T细胞反应性的短暂丧失,如IL-2的产生。

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