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Critical influence of natural regulatory CD25+ T cells on the fate of allografts in the absence of immunosuppression.

机译:在没有免疫抑制的情况下,天然调节性CD25 + T细胞对同种异体移植物命运的关键影响。

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摘要

BACKGROUND: Allografts are occasionally accepted in the absence of immunosuppression. Because naturally occurring CD4(+)CD25(+) regulatory T cells (natural CD25(+) Treg cells) have been shown to inhibit allograft rejection, we investigated their influence on the outcome of allografts in nonimmunosuppressed mouse recipients. METHODS: We compared survival times of male CBA/Ca skin grafts in female CBA/Ca recipients expressing a transgenic anti-HY T-cell receptor on a RAG-1(+/+) (A1[M]RAG+) or a RAG-1(-/-) (A1[M]RAG-) background. Depletion of natural CD25(+) Treg cells in A1[M]RAG+ mice was achieved by in vivo administration of the PC61 monoclonal antibody. The influence of natural CD25(+) Treg cells on the fate of major histocompatibility complex class II-mismatched (C57BL/6X bm12)F1 skin or bm12 heart transplants in C57BL/6 recipients was also assessed. Finally, we investigated the impact of natural CD25(+) Treg cells on the production of T-helper (Th)1 and Th2 cytokines in mixed lymphocyte cultures between C57BL/6 CD4(+) CD25(-) T cells as responders and bm12 or (C57BL/6X bm12)F1 antigen-presenting cells as stimulators. RESULTS: Male allografts were spontaneously accepted by female A1(M)RAG+ mice but readily rejected by female A1(M)RAG+ mice depleted of natural CD25(+) Treg cells by pretreatment with the PC61 monoclonal antibody. Depletion of CD25(+) Treg cells also enhanced eosinophil-determined rejection of (C57BL/6X bm12)F1 skin grafts or bm12 cardiac grafts in C57BL/6 recipients. Finally, natural CD25(+) Treg cells inhibited the production of interleukin (IL)-2, interferon-gamma, IL-5, and IL-13 in mixed lymphocyte culture in a dose-dependent manner. CONCLUSION: Natural CD25(+) Treg cells control Th1- and Th2-type allohelper T-cell responses and thereby influence the fate of allografts in nonimmunosuppressed recipients.
机译:背景:在缺乏免疫抑制的情况下,偶尔接受同种异体移植。因为已显示天然存在的CD4(+)CD25(+)调节性T细胞(天然CD25(+)Treg细胞)抑制同种异体移植排斥,所以我们研究了它们对同种异体移植在非免疫抑制小鼠受体中的影响。方法:我们比较了在RAG-1(+ / +)(A1 [M] RAG +)或RAG-上表达转基因抗HY T细胞受体的雌性CBA / Ca受体中雄性CBA / Ca皮肤移植物的存活时间。 1(-/-)(A1 [M] RAG-)背景。通过体内施用PC61单克隆抗体可实现对A1 [M] RAG +小鼠体内天然CD25(+)Treg细胞的消耗。还评估了天然CD25(+)Treg细胞对C57BL / 6受体中主要组织相容性复杂的II类不匹配(C57BL / 6X bm12)F1皮肤或bm12心脏移植的命运的影响。最后,我们研究了天然CD25(+)Treg细胞对作为应答者的C57BL / 6 CD4(+)CD25(-)T细胞和bm12之间混合淋巴细胞培养物中T辅助(Th)1和Th2细胞因子产生的影响。或(C57BL / 6X bm12)F1抗原呈递细胞作为刺激物。结果:雄性同种异体移植被雌性A1(M)RAG +小鼠自然接受,但通过PC61单克隆抗体预处理,被天然CD25(+)Treg细胞耗尽的雌性A1(M)RAG +小鼠轻易拒绝。 CD25(+)Treg细胞的耗竭还增强了C57BL / 6受者的(C57BL / 6X bm12)F1皮肤移植或bm12心脏移植的嗜酸性粒细胞决定的排斥反应。最后,天然CD25(+)Treg细胞以剂量依赖性方式抑制混合淋巴细胞培养物中白介素(IL)-2,干扰素-γ,IL-5和IL-13的产生。结论:天然CD25(+)Treg细胞控制Th1和Th2型同种异体辅助性T细胞反应,从而影响非免疫抑制受体同种异体移植的命运。

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