首页> 外文期刊>British Journal of Haematology >Predominant or complete recipient T-cell chimerism following alemtuzumab-based allogeneic transplantation is reversed by donor lymphocytes and not associated with graft failure
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Predominant or complete recipient T-cell chimerism following alemtuzumab-based allogeneic transplantation is reversed by donor lymphocytes and not associated with graft failure

机译:基于阿仑单抗的同种异体移植后的优势或完全受体T细胞嵌合现象被供体淋巴细胞逆转,与移植失败无关

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The clinical significance of mixed chimerism following allogeneic haematopoietic stem cell transplantation (HSCT) remains controversial. Its relevance and incidence are probably influenced by the conditioning regimen and incorporation of T-cell depletion. The presence of recipient chimerism levels >40-50% following T-cell replete reduced intensity transplantation correlates with a high risk of graft rejection, regardless of donor-lymphocyte infusions, but it is unclear whether this finding translates to T-cell depleted transplants. We conducted a retrospective single-institution analysis of patients receiving alemtuzumab-based HSCT. 27/152 (18%) evaluable cases had predominantly recipient T-cell chimerism at 3months or beyond. By contrast, coincident chimerism in the granulocyte lineage was predominantly of donor origin (median 100%) in all but one patient. Donor lymphocyte infusion effectively converted predominantly recipient T-cell chimerism to ful donor chimerism in all evaluable cases including three cases with no detectable donor T cells. The only graft failure occurred in the patient with predominantly recipient myeloid chimerism in whom rejection occurred rapidly before donor lymphocytes could be administered. We conclude that predominant or complete recipient T-cell chimerism following alemtuzumab-based regimens does not have the same clinical implications as that following T-cell replete transplants and can be effectively converted with donor lymphocytes without the need for lympho-depleting agents or re-conditioning.
机译:异基因造血干细胞移植(HSCT)后混合嵌合体的临床意义仍存在争议。它的相关性和发生率可能受调节方案和T细胞耗竭的影响。 T细胞补充强度降低的移植后,受体嵌合体水平> 40-50%的存在与移植排斥的高风险相关,而与供体淋巴细胞输注无关,但尚不清楚这一发现是否转化为T细胞耗尽的移植。我们对接受基于alemtuzumab的HSCT的患者进行了回顾性单机构分析。可评估的27/152(18%)病例主要在3个月或更长时间内出现受体T细胞嵌合。相比之下,除一名患者外,粒细胞谱系中的同时嵌合主要来自供体来源(中位数为100%)。在所有可评估的病例中,包括三例未检测到供体T细胞的情况下,供体淋巴细胞输注可将主要的受体T细胞嵌合体有效转化为完全供体嵌合体。唯一的移植失败发生在主要为受体髓样嵌合体的患者中,在接受捐赠者淋巴细胞治疗之前,排斥反应迅速发生。我们得出的结论是,基于基于alemtuzumab的治疗方案占优势或完全的受体T细胞嵌合并不具有与T细胞大量移植后相同的临床意义,并且可以用供体淋巴细胞进行有效转化,而无需使用淋巴细胞消耗剂或重新进行。条件。

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