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首页> 外文期刊>American journal of transplantation: official journal of the American Society of Transplantation and the American Society of Transplant Surgeons >iNKT cell activation plus T‐cell transfer establishes complete chimerism in a murine sublethal bone marrow transplant model
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iNKT cell activation plus T‐cell transfer establishes complete chimerism in a murine sublethal bone marrow transplant model

机译:Inkt细胞活化加T细胞转移在鼠核骨髓移植模型中建立了完全的斜切性

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摘要

Transplant tolerance induction makes it possible to preserve functional grafts for a lifetime without immunosuppressants. One powerful method is to generate mixed hematopoietic chimeras in recipients by adoptive transfer of donor‐derived bone marrow cells (BMCs). In our murine transplantation model, we established a novel method for mixed chimera generation using sublethal irradiation, CD40‐CD40L blockade, and invariant natural killer T‐cell activation. However, numerous BMCs that are required to achieve stable chimerism makes it difficult to apply this model for human transplantation. Here, we show that donor‐derived splenic T cells could contribute to not only the reduction of BMC usage but also the establishment of complete chimerism in model mice. By cotransfer of T cells together even with one‐fourth of the BMCs used in our original method, the recipient mice yielded complete chimerism and could acquire donor‐specific skin‐allograft tolerance. The complete chimeric mice did not show any remarks of graft versus host reaction in vivo and in vitro. Inhibition of the apoptotic signal resulted in increase in host‐derived CD8 + T cells and chimerism brake. These results suggest that donor‐derived splenic T cells having veto activity play a role in the depletion of host‐derived CD8 + T cells and the facilitation of complete chimerism.
机译:移植耐受性诱导使得可以在没有免疫抑制剂的情况下保持寿命的功能移植物。一种强大的方法是通过过度转移供体源性骨髓细胞(BMC)来生成受体中的混合造血嵌合体。在我们的小鼠移植模型中,我们建立了一种使用亚致死辐射,CD40-CD40L阻断和不变自然杀伤T细胞活化的混合嵌合生成的新方法。然而,达到稳定的逆变所需的许多BMC使得难以应用这种模型进行人类移植。在这里,我们表明供体衍生的脾脏T细胞不仅可以减少BMC使用的减少,而且还可以为模型小鼠建立完全斜倚的建立。通过T细胞的COT转移即使我们原始方法中使用的四分之一的BMC,受体小鼠也会产生完全的斜切性,并且可以获得施主特异性皮肤 - 同种异体移植耐受性。完整的嵌合小鼠没有显示移植物与体内反应的任何评论。抑制凋亡信号导致宿主衍生的CD8 + T细胞和嵌合体制动器增加。这些结果表明,具有veto活性的供体衍生的脾脏T细胞在宿主衍生的CD8 + T细胞的耗尽中起作用以及完全逆变的促进。

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