首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Inducible costimulator-dependent IL-10 production by regulatory T cells specific for self-antigen.
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Inducible costimulator-dependent IL-10 production by regulatory T cells specific for self-antigen.

机译:通过对自身抗原具有特异性的调节性T细胞诱导可诱导的共刺激物依赖性IL-10产生。

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In this study, we investigated the relationship between the expression levels of self-antigen and the function of self-reactive T cells in the periphery. To this end, we used two rat insulin promoter-ovalbumin (RIP-OVA) transgenic mice (RIP-OVA(high), RIP-OVA(low)) in which was produced only in pancreatic beta-islet cells. The OVA-producing transgenic mice were crossed to DO.11.10 (DO) mice expressing a T cell antigen receptor specific for OVA(323-339). The responsiveness of peripheral CD4(+) T cells in the double transgenic mice was examined. We demonstrated that hyporesponsive but highly IL-10-producing T cells were developed in DO x OVA(high) mice only, not in DO x OVA(low) mice. These IL-10-producing T cells exhibited regulatory activity both in in vitro and in vivo experiments. Moreover, these IL-10-producing regulatory T (Tr) cells expressed high levels of inducible costimulator (ICOS) before in vitro stimulation. Blockade of ICOS-signaling inhibited the production of IL-10 and abrogated the inhibitory function of these Tr cells. Thus, these results suggested that the development of IL-10-producing Tr cells depends on the expression levels of self-antigen in vivo and that ICOS signal plays a critical role in immune regulation by IL-10-producing Tr cells in self-tolerance.
机译:在这项研究中,我们调查了自身抗原的表达水平与周围的自身反应性T细胞功能之间的关系。为此,我们使用了两只仅在胰岛胰岛细胞中产生的大鼠胰岛素启动子-卵清蛋白(RIP-OVA)转基因小鼠(RIP-OVA(高),RIP-OVA(低))。将产生OVA的转基因小鼠与表达对OVA(323-339)具有特异性的T细胞抗原受体的DO.11.10(DO)小鼠杂交。在双转基因小鼠中检查外周CD4(+)T细胞的反应。我们证明低反应性但高产生IL-10的T细胞仅在DO x OVA(低)小鼠中发展,而不在DO x OVA(低)小鼠中发展。这些产生IL-10的T细胞在体外和体内实验中均表现出调节活性。而且,在体外刺激之前,这些产生IL-10的调节性T(Tr)细胞表达高水平的可诱导共刺激物(ICOS)。阻断ICOS信号传导抑制了IL-10的产生,并取消了这些Tr细胞的抑制功能。因此,这些结果表明,产生IL-10的Tr细胞的发育取决于体内自身抗原的表达水平,并且ICOS信号在产生IL-10的Tr细胞的自我耐受中在免疫调节中起关键作用。 。

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