Bodas Manish, Jain Nitya, Awasthi Amit, Martin Sunil, Penke Loka Raghu Kumar, Dandekar Dineshkumar, Mitra Debashis, Saha Bhaskar
National Centre for Cell Science, Ganeshkhind, Maharashtra, Pune 411-007, India.
J Immunol. 2006 Oct 1;177(7):4636-43. doi: 10.4049/jimmunol.177.7.4636.
Leishmania donovani, a protozoan parasite, inflicts a fatal disease, visceral leishmaniasis. The suppression of antileishmanial T cell responses that characterizes the disease was proposed to be due to deficiency of a T cell growth factor, IL-2. We demonstrate that during the first week after L. donovani infection, IL-2 induces IL-10 that suppresses the host-protective functions of T cells 14 days after infection. The observed suppression is concurrent with increased CD4+ glucocorticoid-induced TNF receptor+ T cells and Foxp3 expression in BALB/c mice, implicating IL-2-dependent regulatory T cell control of antileishmanial immune responses. Indeed, IL-2 and IL-10 neutralization at different time points after the infection demonstrates their distinct roles at the priming and effector phases, respectively, and establishes kinetic modulation of ongoing immune responses as a principle of a rational, phase-specific immunotherapy.
杜氏利什曼原虫是一种原生动物寄生虫,可引发致命疾病——内脏利什曼病。该疾病的特征是抗利什曼原虫T细胞反应受到抑制,有人提出这是由于T细胞生长因子白细胞介素-2(IL-2)缺乏所致。我们证明,在杜氏利什曼原虫感染后的第一周,IL-2会诱导产生IL-10,而IL-10会在感染14天后抑制T细胞的宿主保护功能。在BALB/c小鼠中观察到的这种抑制作用与CD4+糖皮质激素诱导的肿瘤坏死因子受体+ T细胞增加以及Foxp3表达增加同时出现,这表明抗利什曼原虫免疫反应受到IL-2依赖性调节性T细胞的控制。事实上,在感染后的不同时间点对IL-2和IL-10进行中和,分别证明了它们在启动阶段和效应阶段的不同作用,并确立了对正在进行的免疫反应进行动力学调节,作为合理的、阶段特异性免疫治疗的原则。
