首页> 外文期刊>The journal of immunology >Role for Thymic and Splenic Regulatory CD4+ T Cells Induced by Donor Dendritic Cells in Allograft Tolerance by LF15-0195 Treatment
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Role for Thymic and Splenic Regulatory CD4+ T Cells Induced by Donor Dendritic Cells in Allograft Tolerance by LF15-0195 Treatment

机译:供体树突状细胞诱导的胸腺和脾脏调节性CD4 + T细胞在LF15-0195处理对同种异体移植耐受中的作用

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A 20-day treatment with LF15-0195, a deoxyspergualine analogue, induced allograft tolerance in a fully MHC-mismatched heart allograft model in the rat. Long-term allografts displayed minimal cell infiltration with no signs of chronic rejection. CD4+ spleen T cells from tolerant LF15-0195-treated recipients were able to suppress in vitro proliferation of allogeneic CD4+ T cells and to transfer tolerance to second syngeneic recipients, demonstrating dominant suppression by regulatory cells. A significant increase in the percentage of CD4+CD25+ T cells was observed in the thymus and spleen from tolerant LF15-0195-treated recipient. In vitro direct stimulation with donor APCs demonstrated that CD4+ regulatory T cells proliferated weakly and expressed low levels of IFN-γ, IL-10, and IL-2. CD4+CD25+ cell depletion increased IL-2 production by CD4+CD25? thymic cells, but not splenic cells. Moreover, tolerance was transferable with splenic and thymic CD4+CD25+ cells, but also in 50% of cases with splenic CD4+CD25? cells, demonstrating that CD25 can be a marker for regulatory cells in the thymus, but not in the periphery. In addition, we presented evidences that donor APCs were required to induce tolerance and to expand regulatory CD4+ T cells. This study demonstrates that LF15-0195 treatment induces donor APCs to expand powerful regulatory CD4+CD25+/? T cells present in both the central and peripheral compartments.
机译:在完全MHC不匹配的心脏同种异体移植模型中,用LF15-0195(一种脱氧精油类似物)进行20天的治疗可诱导同种异体移植耐受。长期同种异体移植显示出最小的细胞浸润,没有慢性排斥的迹象。来自耐受性LF15-0195处理的接受者的CD4 +脾T细胞能够抑制同种CD4 + T细胞的体外增殖,并将耐受性转移至第二同系接受者,证明了调节细胞的显性抑制。在耐受性LF15-0195处理的接受者的胸腺和脾脏中观察到CD4 + CD25 + T细胞百分比的显着增加。用供体APC进行的体外直接刺激证明CD4 +调节性T细胞增殖较弱,并表达低水平的IFN-γ,IL-10和IL-2。 CD4 + CD25 +细胞耗竭会增加CD4 + CD25产生的IL-2?胸腺细胞,但不是脾细胞。而且,脾脏和胸腺CD4 + CD25 +细胞的耐受性是可以转移的,但脾脏CD4 + CD25 +的病例中也有50%可以耐受。这表明CD25可以作为胸腺中而非外周细胞中调控细胞的标志物。此外,我们提供的证据表明,需要供体APC诱导耐受性并扩展调节性CD4 + T细胞。这项研究表明,LF15-0195处理可诱导供体APC扩展功能强大的调节性CD4 + CD25 + /? T细胞既存在于中央区室,也存在于周边区室。

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