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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Efficient Induction of Primary and Secondary T Cell-Dependent Immune Responses In Vivo in the Absence of Functional IL-2 and IL-15 Receptors.
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Efficient Induction of Primary and Secondary T Cell-Dependent Immune Responses In Vivo in the Absence of Functional IL-2 and IL-15 Receptors.

机译:在缺乏功能性IL-2和IL-15受体的情况下有效诱导初级和次级T细胞依赖性免疫反应。

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摘要

IL-2 and IL-15 are thought to be important cytokines for T cell-dependent immune responses. Mice deficient in IL-2, IL-2Ralpha, and IL-2Rbeta are each characterized by a rapid lethal autoimmune lymphoproliferative disorder that complicates their use in studies aimed at investigating the role of these cytokines and receptors for immune responses in vivo. We have previously characterized a novel transgenic (Tg) mouse on the IL-2Rbeta(-/-) genetic background (Tg(-/-) mice) that lacks autoimmune disease but still contains peripheral T cells that are nonresponsive to IL-2 and IL-15. In the present study, these mice were used to investigate the extent by which IL-2 and IL-15 are essential for T cell immunity in vivo. Tg(-/-) mice generated near normal primary and secondary Ab responses to OVA, readily mounted first and second set allogeneic skin graft rejection responses, and developed primary and recall CD8 T cell responses to vaccinia virus. However, Tg(-/-) mice generated a slightly lower level of IgG2a Abs to OVA, exhibited a somewhat delayed first set skin graft rejection response with lower allo-specific CTL, and developed a significantly lower number of IFN-gamma-producing vaccinia-specific CD8(+) T cells. Thus, although T effector function is somewhat impaired, T cell immunity is largely functional in the absence of IL-2- and IL-15-induced signaling through IL-2Rbeta.
机译:IL-2和IL-15被认为是依赖T细胞的免疫反应的重要细胞因子。缺乏IL-2,IL-2Ralpha和IL-2Rbeta的小鼠均以快速致命的自身免疫性淋巴组织增生性疾病为特征,这使它们在旨在研究这些细胞因子和受体在体内免疫反应中的作用的研究中的用途复杂化。我们先前已在缺乏自身免疫性疾病但仍包含对IL-2和TC无效的外周T细胞的IL-2Rbeta(-/-)遗传背景上表征了新型转基因(Tg)小鼠(Tg(-/-)小鼠)。 IL-15。在本研究中,这些小鼠用于研究IL-2和IL-15对体内T细胞免疫至关重要的程度。 Tg(-/-)小鼠产生了对OVA的正常原发性和继发性Ab反应,易于安装第一组和第二组同种异体皮肤移植排斥反应,并发展了对牛痘病毒的原发和召回CD8 T细胞应答。但是,Tg(-/-)小鼠产生的OVA IgG2a Abs含量略低,显示出的第一组皮肤移植排斥反应有所延迟,同种异体特异性CTL较低,并且产生IFN-γ的牛痘明显减少特异的CD8(+)T细胞。因此,尽管T效应子功能有些受损,但是在不存在通过IL-2Rβ通过IL-2和IL-15诱导的信号传导的情况下,T细胞免疫在很大程度上起作用。

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