首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Co-transplantation of pure blood stem cells with antigen-specific but not bulk T cells augments functional immunity
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Co-transplantation of pure blood stem cells with antigen-specific but not bulk T cells augments functional immunity

机译:纯血干细胞与抗原特异性但不与大量T细胞共移植可增强功能性免疫

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摘要

Impaired immunity is a fundamental obstacle to successful allogeneic hematopoietic cell transplantation. Mature graft T cells are thought to provide protection from infections early after transplantation, but can cause life-threatening graft-vs.-host disease. Human CMV is a major pathogen after transplantation. We studied reactivity against the mouse homologue, murine CMV (MCMV), in lethally irradiated mice given allogeneic purified hematopoietic stem cells (HSCs) or HSCs supplemented with T cells or T-cell subsets. Unexpectedly, recipients of purified HSCs mounted superior antiviral responses compared with recipients of HSC plus unselected bulk T cells. Furthermore, supplementation of purified HSC grafts with CD8+ memory or MCMV-specific T cells resulted in enhanced antiviral reactivity. Posttransplantation lymphopenia promoted massive expansion of MCMV-specific, T cells when no competing donor T cells were present. In recipients of pure HSCs, naive and memory T cells and innate lymphoid cell populations developed. In contrast, the lymphoid pool in recipients of bulk T cells was dominated by effector memory cells. These studies show that pure HSC transplantations allow superior protective immunity against a viral pathogen compared with unselected mature T cells. This reductionist transplant model reveals the impact of graft composition on regeneration of host, newly generated, and mature transferred T cells, and underscores the deleterious effects of bulk donor T cells. Our findings lead us to conclude that grafts composed of purified HSCs provide an optimal platform for in vivo expansion of selected antigen-specific cells while allowing the reconstitution of a naive T-cell pool.
机译:免疫力受损是异基因造血细胞成功移植的根本障碍。人们认为成熟的移植T细胞可在移植后早期提供保护,防止感染,但会导致危及生命的移植物抗宿主病。人CMV是移植后的主要病原体。我们研究了给予同种异体纯化的造血干细胞(HSC)或补充了T细胞或T细胞亚群的HSC的致死性辐射小鼠的抗小鼠同源物鼠CMV(MCMV)的反应性。出乎意料的是,与HSC加上未选择的大量T细胞的接受者相比,纯化的HSC的接受者表现出更高的抗病毒反应。此外,用CD8 +记忆或MCMV特异性T细胞补充纯化的HSC移植物可增强抗病毒反应性。当不存在竞争性供体T细胞时,移植后淋巴细胞减少促进MCMV特异性T细胞的大规模扩增。在纯HSC的受体中,幼稚和记忆T细胞和先天性淋巴样细胞群得以发展。相反,散装T细胞受体中的淋巴池由效应记忆细胞决定。这些研究表明,与未选择的成熟T细胞相比,单纯的HSC移植可对病毒病原体提供优异的保护性免疫。该还原剂移植模型揭示了移植物成分对宿主,新生成的和成熟转移的T细胞再生的影响,并强调了大量供体T细胞的有害作用。我们的发现使我们得出结论,由纯化的HSC组成的移植物为体内扩增选定的抗原特异性细胞提供了一个最佳平台,同时允许重组天然T细胞池。

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