McRae B L, Semnani R T, Hayes M P, van Seventer G A
Department of Pathology, University of Chicago, IL 60637, USA.
J Immunol. 1998 May 1;160(9):4298-304.
We have investigated the role of type I IFNs (IFN-alpha and -beta) in human T cell differentiation using anti-CD3 mAb and allogeneic, in vitro-derived dendritic cells (DC) as APCs. DC were very efficient activators of naive CD4+ T cells, providing necessary costimulation and soluble factors to support Th1 differentiation and expansion. Addition of IFN-alphabeta to DC/T cell cultures resulted in induction of T cell IL-10 production and inhibition of IFN-gamma, TNF-alpha, and LT secretion. Diminished T cell IFN-gamma production correlated with IFN-alphabeta-mediated inhibition of the p40 chain of the IL-12 heterodimer secreted by DC. Suppression of p40 IL-12 and IFN-gamma was not due to increased levels of IL-10 in these cultures, and production of IFN-gamma could be restored by exogenous IL-12. These data indicate that type I IFNs inhibit DC p40 IL-12 expression, which is required for development of IFN-gamma-producing CD4+ T cells. Furthermore, when T cells were restimulated without IFN-beta, these cells induced less p40 IL-12 from DC, suggesting that the functional properties of T cells may regulate DC function. Thus, IFN-alphabeta inhibits both IL-12-dependent and independent Th1 cytokine production and provides a mechanism for inhibition of IL-12-mediated immunity in viral infections.
我们使用抗CD3单克隆抗体以及体外培养的同种异体树突状细胞(DC)作为抗原呈递细胞(APC),研究了I型干扰素(IFN-α和 -β)在人T细胞分化中的作用。DC是未成熟CD4+ T细胞非常有效的激活剂,可提供必要的共刺激和可溶性因子以支持Th1细胞的分化和扩增。向DC/T细胞培养物中添加IFN-αβ可诱导T细胞产生IL-10,并抑制IFN-γ、TNF-α和淋巴毒素(LT)的分泌。T细胞IFN-γ产生的减少与IFN-αβ介导的DC分泌的IL-12异二聚体p40链的抑制有关。p40 IL-12和IFN-γ的抑制并非由于这些培养物中IL-10水平的升高,外源性IL-12可恢复IFN-γ的产生。这些数据表明,I型干扰素抑制DC p40 IL-12的表达,而这是产生IFN-γ的CD4+ T细胞发育所必需的。此外,当T细胞在没有IFN-β的情况下再次受到刺激时,这些细胞诱导DC产生的p40 IL-12减少,这表明T细胞的功能特性可能调节DC的功能。因此,IFN-αβ抑制依赖IL-12和不依赖IL-12的Th1细胞因子的产生,并为病毒感染中抑制IL-12介导的免疫提供了一种机制。
