Lopes M F, Nunes M P, Henriques-Pons A, Giese N, Morse H C, Davidson W F, Araújo-Jorge T C, DosReis G A
Programa de Immunobiologia, Instituto de Biofisica Carlos Chagas Filho, Universidade Federal do Rio de Janeiro, RJ, Brasil.
Eur J Immunol. 1999 Jan;29(1):81-9. doi: 10.1002/(SICI)1521-4141(199901)29:01<81::AID-IMMU81>3.0.CO;2-Y.
Infection of BALB/c mice with Trypanosoma cruzi resulted in up-regulated expression of Fas and Fas ligand (FasL) mRNA by splenic CD4+ T cells, activation-induced CD4+ T cell death (AICD), and in Fas: FasL-mediated cytotoxicity. When CD4+ T cells from infected mice were co-cultured with T. cruzi-infected macrophages, onset of AICD exacerbated parasite replication. CD4+ T cells from T. cruzi-infected FasL-deficient BALB gld/gld mice had no detectable AICD in vitro and their activation with anti-TCR did not exacerbate T. cruzi replication in macrophages. However, infection of BALB gld/gld mice with T. cruzi resulted in higher and more prolonged parasitemia, compared to wild-type mice. Secretion of Th2 cytokines IL-10 and IL-4 by CD4+ T cells from infected gld mice was markedly increased, compared to controls. In addition, in vivo injection of anti-IL-4 mAb, but not of an isotype control mAb, reduced parasitemia in both gld and wild-type mice. These results indicate that, besides controlling CD4+ T cell AICD and parasite replication in vitro, an intact Fas: FasL pathway also controls the host cytokine response to T. cruzi infection in vivo, being required to prevent an exacerbated Th2-type immune response to the parasite.
用克氏锥虫感染BALB/c小鼠会导致脾脏CD4+ T细胞中Fas和Fas配体(FasL)mRNA表达上调、激活诱导的CD4+ T细胞死亡(AICD)以及Fas:FasL介导的细胞毒性。当将感染小鼠的CD4+ T细胞与感染克氏锥虫的巨噬细胞共培养时,AICD的发生会加剧寄生虫的复制。来自感染克氏锥虫的FasL缺陷型BALB gld/gld小鼠的CD4+ T细胞在体外未检测到AICD,并且用抗TCR激活它们不会加剧巨噬细胞中克氏锥虫的复制。然而,与野生型小鼠相比,用克氏锥虫感染BALB gld/gld小鼠会导致更高且更持久的寄生虫血症。与对照组相比,感染gld小鼠的CD4+ T细胞分泌的Th2细胞因子IL-10和IL-4明显增加。此外,体内注射抗IL-4单克隆抗体而非同型对照单克隆抗体可降低gld和野生型小鼠的寄生虫血症。这些结果表明,除了在体外控制CD4+ T细胞AICD和寄生虫复制外,完整的Fas:FasL途径还在体内控制宿主对克氏锥虫感染的细胞因子反应,这对于防止对寄生虫的Th2型免疫反应加剧是必需的。
