Taylor-Robinson A W, Phillips R S
Wellcome Laboratories for Experimental Parasitology, University of Glasgow, U.K.
Immunology. 1992 Sep;77(1):99-105.
Protective immunity to asexual malaria parasites appears to be mediated predominantly by the CD4+ subset of T lymphocytes. To examine the role of this T-cell population in the immune response to the murine malaria parasite Plasmodium chabaudi, CD4+ clones derived from infected mice were raised and propagated in vitro. Analysis of the reactivity of clones responsive to parasite antigen demonstrated that the CD4+ cell response is heterogeneous and is consistent with the idea of two functionally distinct CD4+ subsets. Those populations derived early during primary infection secreted interleukin-2 (IL-2) and interferon-gamma (IFN-gamma) upon antigenic stimulation in vitro, i.e. they had a cytokine repertoire typical of the delayed-type inflammatory T-helper 1 (Th1) CD4+ subset. In contrast, cells taken after clearance of a secondary infection produced IL-4 and acted as effective helper cells for anti-malarial antibody (Ab) synthesis in vitro, and thereby had the characteristics of Th2 cells. The appearance in vivo of Th1 and then Th2 clones specific for P. chabaudi-parasitized erythrocytes (pRBC) supports the proposal from limiting culture analyses that for this malaria parasite resolution of primary parasitaemia is predominantly through the action of cytokines rather than Ab, and that final clearance requires helper cells and specific immunoglobulin.
对无性疟原虫的保护性免疫似乎主要由T淋巴细胞的CD4 +亚群介导。为了研究该T细胞群体在对鼠疟原虫查巴迪疟原虫免疫反应中的作用,从感染小鼠中获得的CD4 +克隆在体外培养和增殖。对寄生虫抗原反应性克隆的反应性分析表明,CD4 +细胞反应是异质性的,这与两个功能不同的CD4 +亚群的观点一致。那些在初次感染早期产生的群体在体外抗原刺激后分泌白细胞介素-2(IL-2)和干扰素-γ(IFN-γ),即它们具有典型的迟发型炎性T辅助1(Th1)CD4 +亚群的细胞因子谱。相反,在二次感染清除后获取的细胞产生IL-4,并在体外作为抗疟抗体(Ab)合成的有效辅助细胞,因此具有Th2细胞的特征。针对查巴迪疟原虫寄生红细胞(pRBC)的Th1和Th2克隆在体内的出现支持了有限培养分析的提议,即对于这种疟原虫,初次寄生虫血症的消退主要是通过细胞因子的作用而不是Ab,并且最终清除需要辅助细胞和特异性免疫球蛋白。
