Centre for Immunology & Infection, Hull York Medical School and Department of Biology, University of York, York, United Kingdom.
PLoS Pathog. 2012;8(7):e1002827. doi: 10.1371/journal.ppat.1002827. Epub 2012 Jul 26.
IL-10 is a critical regulatory cytokine involved in the pathogenesis of visceral leishmaniasis caused by Leishmania donovani and clinical and experimental data indicate that disease progression is associated with expanded numbers of CD4⁺ IFNγ⁺ T cells committed to IL-10 production. Here, combining conditional cell-specific depletion with adoptive transfer, we demonstrate that only conventional CD11c(hi) DCs that produce both IL-10 and IL-27 are capable of inducing IL-10-producing Th1 cells in vivo. In contrast, CD11c(hi) as well as CD11c(int/lo) cells isolated from infected mice were capable of reversing the host protective effect of diphtheria toxin-mediated CD11c⁺ cell depletion. This was reflected by increased splenomegaly, inhibition of NO production and increased parasite burden. Thus during chronic infection, multiple CD11c⁺ cell populations can actively suppress host resistance and enhance immunopathology, through mechanisms that do not necessarily involve IL-10-producing Th1 cells.
IL-10 是一种关键的调节性细胞因子,参与了由利什曼原虫引起的内脏利什曼病的发病机制,临床和实验数据表明,疾病的进展与扩增的 CD4⁺IFNγ⁺T 细胞数量有关,这些细胞致力于产生 IL-10。在这里,我们通过条件性细胞特异性耗竭与过继转移相结合,证明只有同时产生 IL-10 和 IL-27 的常规 CD11c(hi)DC 才能在体内诱导产生 IL-10 的 Th1 细胞。相比之下,从感染小鼠中分离出的 CD11c(hi)和 CD11c(int/lo)细胞能够逆转白喉毒素介导的 CD11c⁺细胞耗竭对宿主的保护作用。这反映在脾肿大增加、NO 产生抑制和寄生虫负荷增加。因此,在慢性感染期间,多种 CD11c⁺细胞群可以通过不涉及产生 IL-10 的 Th1 细胞的机制,主动抑制宿主的抵抗力并增强免疫病理学。
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