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首页> 外文期刊>Chimerism >Mixed chimerism evolution is associated with T regulatory type 1 (Trl) cells in a beta-thalassemic patient after haploidentical haematopoietic stem cell transplantation
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Mixed chimerism evolution is associated with T regulatory type 1 (Trl) cells in a beta-thalassemic patient after haploidentical haematopoietic stem cell transplantation

机译:异型造血干细胞移植后β-地中海贫血患者中混合嵌合体进化与T调节型1(Trl)细胞相关

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摘要

In a cohort of p-Thalassemia (p-Thal) transplanted with haploidentical-HSCT we identified one transplanted patient characterized by persistent mixed chimerism (PMC) for several months after HSCT. In this unique B-Thal patient we assessed the donor engraftment overtime after transplantation, the potential loss of the non-shared HLA haplotype, and the presence of CD49b+LAG-3+ T regulatory type 1 (Tr1) cells, previously demonstrated to be associated with PMC after HLA-related HSCT for B-Thal. The majority of the patient's erythrocytes were of donor origin, whereas T cells were initially mostly derived from the recipient, no HLA loss, but an increased frequency of circulating Trl cells were observed. For the first time, we showed that when the proportion of residual donor cells decreases, the frequency of CD49b+LAG-3+ Tr1 cells declines, reaching the levels present in healthy subjects. These findings confirm previous results obtained in transplant related settings for (3-Thal, and supported the centralrole of Trl cells in promoting and maintaining PMC after allo-HSCT.
机译:在单倍体HSCT移植的p-地中海贫血(p-Thal)队列中,我们鉴定出一名移植患者,其特征为HSCT后数月持续混合嵌合体(PMC)。在这例独特的B-Thal患者中,我们评估了移植后供体植入的超时情况,非共有HLA单倍型的潜在丧失以及以前证明的CD49b + LAG-3 + T调节型1(Tr1)细胞的存在。 B-Thal的HLA相关HSCT后与PMC相关。患者的大多数红细胞是供体来源的,而T细胞最初主要来自受体,没有HLA丢失,但观察到循环Trl细胞的频率增加。首次显示,当残留供体细胞的比例降低时,CD49b + LAG-3 + Tr1细胞的频率降低,达到健康受试者的水平。这些发现证实了在(3-Thal)的移植相关设置中获得的先前结果,并支持了异体-HSCT后Tr1细胞的中枢在促进和维持PMC中的作用。

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