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首页> 外文期刊>American Journal of Transplantation >B Cell Repopulation After Alemtuzumab Induction—Transient Increase in Transitional B Cells and Long-Term Dominance of Na?ve B Cells
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B Cell Repopulation After Alemtuzumab Induction—Transient Increase in Transitional B Cells and Long-Term Dominance of Na?ve B Cells

机译:Alemtuzumab诱导后B细胞重新聚集-过渡性B细胞的短暂增加和幼稚B细胞的长期优势

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摘要

In organ transplantation, the composition of the B-cell compartment is increasingly identified as an important determinant for graft outcome. Whereas na?ve and transitional B cells have been associated with long-term allograft survival and operational tolerance, memory B cells have been linked to decreased allograft survival. Alemtuzumab induction therapy effectively depletes B cells, but is followed by rapid repopulation up to levels exceeding base line. The characteristics of the repopulating B cells are currently unknown. We studied the phenotypic and functional characteristics of B cells longitudinally in 19 kidney transplant recipients, before and at 6, 9 and 12 months after alemtuzumab induction therapy. A transient increase in transitional B cells and cells with phenotypic characteristics of regulatory B cells, as well as a long-term dominance in na?ve B cells was found in alemtuzumab-treated kidney transplant recipients, which was not influenced by conversion from tacrolimus to sirolimus. At all time-points after treatment, B cells showed unaltered proliferative and IgM-producing capacity as compared to pretransplant samples, whereas the ability to produce IgG was inhibited long-term. In conclusion, induction therapy with alemtuzumab results in a long-term shift toward na?ve B cells with altered phenotypic and functional characteristics.
机译:在器官移植中,越来越多地将B细胞区室的组成确定为移植结果的重要决定因素。幼稚和过渡性B细胞与长期同种异体移植存活率和操作耐受性有关,而记忆B细胞则与同种异体移植物存活率下降相关。 Alemtuzumab诱导疗法可有效消耗B细胞,但随后迅速重新繁殖,直至超过基线水平。目前尚不清楚重聚B细胞的特征。我们在19例肾移植受者中,在Alemtuzumab诱导治疗之前和之后6、9和12个月纵向研究了B细胞的表型和功能特征。在用阿来珠单抗治疗的肾脏移植受者中发现过渡性B细胞和具有调节性B细胞表型特征的细胞短暂增加,并且在幼稚B细胞中长期处于优势地位,这不受他克莫司转化为肾上腺素的影响西罗莫司。在治疗后的所有时间点上,与移植前样品相比,B细胞均显示出不变的增殖能力和IgM产生能力,而长期产生IgG的能力受到抑制。总之,用阿仑单抗的诱导疗法导致长期向具有改变的表型和功能特征的幼稚B细胞转移。

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