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Transplantation: Factors governing the activation of adoptively transferred donor T cells infused after allogeneic bone marrow transplantation in the mouse

机译:移植:控制异基因骨髓移植后注入的过继转移供体T细胞活化的因素

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摘要

Murine models of bone marrow transplantation were used to study the mechanisms governing the activation of donor lymphocyte infusions (DLIs) manifesting as lymphohematopoietic graft-versus-host (LH-GVH) and graft-versus-leukemia (GVL) reactivities. We demonstrate here that established mixed chimerism influences the potency of DLI-mediated alloreactivity only in the MHC-mismatched but not MHC-matched setting. In the MHC-matched setting, high levels (≥ 40%) of residual host chimerism correlated negatively with DLI-mediated alloreactivity irrespective of the timing of their administration, the donor's previous sensitization to host antigens, or the level of residual host APCs. In vivo administration of Toll-like receptor (TLR) ligands was required to maximize DLI-mediated LH-GVH and GVL reactivities in chimeras with low levels (≤ 15%) of residual host chimerism. In contrast, coadministration of DLI with antigen-presenting cell (APC) activators was insufficient to augment their LH-GVH response in the presence of high levels of host chimerism unless the host's T cells were transiently depleted. Together, these results show the cardinal influence of donor-host incompatibility on DLI-mediated GVH responses and suggest that in MHC-matched chimeras, the induction of optimal alloreactivity requires not only donor T cells and host APCs but also TLR ligands and in the presence of high levels of host chimerism depletion of host T cells.
机译:小鼠骨髓移植模型用于研究控制供体淋巴细胞输注(DLI)活化的机制,这些机制表现为淋巴造血移植物抗宿主(LH-GVH)和移植物抗白血病(GVL)反应性。我们在这里证明已建立的混合嵌合体仅在MHC不匹配但不MHC匹配的环境中影响DLI介导的同种异体反应的效力。在MHC匹配的环境中,高水平(≥40%)的残余宿主嵌合体与DLI介导的同种反应性呈负相关,而与给药时间,供体先前对宿主抗原的敏化程度或残余宿主APC的水平无关。需要Toll样受体(TLR)配体的体内给药,以最大程度地降低残基嵌合体水平(≤15%)的嵌合体中DLI介导的LH-GVH和GVL反应性。相反,在宿主嵌合体水平高的情况下,除非宿主的T细胞被瞬时耗尽,否则DLI与抗原呈递细胞(APC)激活剂的共同给药不足以增强其LH-GVH反应。总之,这些结果显示了供体-宿主不相容性对DLI介导的GVH反应的主要影响,并表明在MHC匹配的嵌合体中,诱导最佳的同种异体反应不仅需要供体T细胞和宿主APC,而且还需要TLR配体。高水平的宿主嵌合体耗竭宿主T细胞。

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