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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Induction of tolerance-inducing antigen-presenting cells in bone marrow cultures in vitro using monoclonal antibodies to cd200r.
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Induction of tolerance-inducing antigen-presenting cells in bone marrow cultures in vitro using monoclonal antibodies to cd200r.

机译:使用针对cd200r的单克隆抗体体外诱导骨髓培养物中的诱导耐受性的抗原呈递细胞。

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CD200 to CD200R interactions produce immunoregulation. We investigated whether the expression of CD200R on dendritic cell (DC) precursors affects their developmental fate. C57BL/6 bone marrow (BM) cells were cultured in vitro in the presence of (interleukin-4 + granulocyte-macrophage colony-stimulating activity) to generate allostimulatory DCs, which were in turn used to induce cytotoxic T-lymphocyte and cytokine production after culture with C3H responder spleen cells. Some marrow cultures included anti-CD200R antibodies. The inclusion of monoclonal antibodies in different isoforms of CD200R in the BM culture led to a generation of cells (tolerogenic DCs) that were unable to produce allostimulation in vitro with responder cells. Cells taken from these latter mixed leukocyte cultures (MLCs) now contained CD4CD25 cells able to inhibit the antigen-specific MLC response of fresh C3H responder cells to stimulation with C57BL/6 cells, but not stimulation with BALB/c cells. Tolerogenic DCs, infused in vivo into mice receiving C57BL/6 skin grafts, produced antigen-specific decreased rejection of BL/6 allografts, not BALB/c allografts, compared with mice receiving control DCs (generated from BM in the absence of anti-CD200R). The induction of CD4CD25 suppressor cells in MLCs using tolerogenic DCs from the initial BM cultures could be overcome by using limiting numbers of tolerogenic DCs and an excess of allostimulatory DCs derived from BM cultures maintained in the absence of anti-CD200R. These data indicate that anti-CD200R biases stem cells in BM toward the development of suppressive antigen-presenting cells, which can induce CD4CD25 regulatory T cells. Tolerogenic DCs have the potential to modify graft acceptance in vivo.
机译:CD200到CD200R的相互作用产生免疫调节。我们调查了CD200R在树突状细胞(DC)前体上的表达是否影响其发育命运。在(白介素4 +粒细胞巨噬细胞集落刺激活性)存在下体外培养C57BL / 6骨髓(BM)细胞以产生同种异体刺激DC,这些DC继而用于诱导细胞毒性T淋巴细胞和细胞因子的产生C3H反应者脾细胞培养。一些骨髓培养物包括抗CD200R抗体。在BM培养物中CD200R的不同同种型中包含单克隆抗体会导致一代细胞(致耐受性DC)产生,这些细胞无法在体外与应答细胞产生同种刺激。现在,从这些后来的混合白细胞培养物中提取的细胞包含CD4CD25细胞,它们能够抑制新鲜的C3H应答细胞对C57BL / 6细胞刺激的抗原特异性MLC反应,但对BALB / c细胞的刺激却不起作用。与接受对照DC的小鼠(由不存在抗CD200R的BM产生的小鼠)相比,将耐受性DC体内注入到接受C57BL / 6皮肤移植的小鼠体内,可产生抗原特异性降低的BL / 6同种异体移植物(而非BALB / c同种异体移植物)排斥)。可以通过使用有限数量的致耐受性DC和在不存在抗CD200R的情况下维持的过量的源自BM培养物的同种刺激DC来克服使用最初BM培养物中的致耐受性DC诱导MLC中CD4CD25抑制细胞的诱导。这些数据表明,抗CD200R使BM中的干细胞偏向抑制性抗原呈递细胞的发展,后者可诱导CD4CD25调节性T细胞。致耐受性DC具有改变体内移植物接受度的潜力。

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