The persistence of human autoimmune diseases is thought to be mediated predominantly by memory T cells. We investigated the phenotype and migration of memory versus effector T cells in vivo in experimental autoimmune encephalomyelitis (EAE). We found that memory CD4(+) T cells up-regulated the activation marker CD44 as well as CXCR3 and ICOS, proliferated more and produced more interferon-gamma and less interleukin-17 compared to effector T cells. Moreover, adoptive transfer of memory T cells into T cell receptor (TCR)alphabeta(-/-) recipients induced more severe disease than did effector CD4(+) T cells with marked central nervous system inflammation and axonal damage. The uniqueness of disease mediated by memory T cells was confirmed by the differential susceptibility to immunomodulatory therapies in vivo. CD28-B7 T cell costimulatory signal blockade by CTLA4Ig suppressed effector cell-mediated EAE but had minimal effects on disease induced by memory cells. In contrast, ICOS-B7h blockade exacerbated effector T cell-induced EAE but protected from disease induced by memory T cells. However, blockade of the OX40 (CD134) costimulatory pathway ameliorated disease mediated by both memory and effector T cells. Our data extend the understanding of the pathogenicity of autoreactive memory T cells and have important implications for the development of novel therapies for human autoimmune diseases.
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机译:人类自身免疫性疾病的持续存在被认为主要由记忆T细胞介导。我们研究了实验性自身免疫性脑脊髓炎 (EAE) 中体内记忆与效应 T 细胞的表型和迁移。我们发现,与效应 T 细胞相比,记忆 CD4(+) T 细胞上调激活标志物 CD44 以及 CXCR3 和 ICOS,增殖更多,产生更多的干扰素-γ 和更少的白细胞介素-17。此外,记忆 T 细胞过继性转移到 T 细胞受体 (TCR)字母 (-/-) 受体中比效应 CD4(+) T 细胞诱导更严重的疾病,具有明显的中枢神经系统炎症和轴突损伤。记忆T细胞介导的疾病的独特性通过体内免疫调节疗法的差异易感性得到证实。CTLA4Ig阻断CD28-B7 T细胞共刺激信号可抑制效应细胞介导的EAE,但对记忆细胞诱导的疾病影响最小。相比之下,ICOS-B7h 阻断加剧了效应 T 细胞诱导的 EAE,但对记忆 T 细胞诱导的疾病有保护作用。然而,阻断 OX40 (CD134) 共刺激通路可改善由记忆和效应 T 细胞介导的疾病。我们的数据扩展了对自身反应性记忆T细胞致病性的认识,并对人类自身免疫性疾病新疗法的开发具有重要意义。
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