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Long-term immune deficiency after allogeneic stem cell transplantation: B-cell deficiency is associated with late infections

机译:同种异体干细胞移植后的长期免疫缺陷:B细胞缺陷与晚期感染有关

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摘要

Immune reconstitution was analyzed in 140 consecutive patients who were 2-year disease-free and who underwent myeloablative allogeneic transplantation. A CD4 and CD8 defect was observed involving naive, terminally differentiated, memory and competent cells and above limits values for activated subsets. Natural killer cells normalize at six months while we observed expansion of CD19+/CD5+ B cells after three months and a persisting defect of memory B cells. Chronic graft-versus-host disease did not influence significantly those parameters for CD8 subsets while the naïve and competent CD4 subsets were strongly affected. But the most profound impact of chronic graft-versus-host disease was on B-cell subsets, especially on the memory B population. The cumulative incidence of late severe infections was low (14% at four years). Using Cox’s models, only low B-cell counts at 12 (P=0.02) and 24 (P=0.001) months were associated with the hazard of developing late infection, in particular if patients did not develop chronic graft-versus-host disease.
机译:分析了140名连续2年无病且接受清髓同种异体移植的患者的免疫重建。观察到CD4和CD8缺陷,涉及幼稚的,终末分化的,记忆和感受态细胞,并且高于激活子集的极限值。天然杀伤细胞在六个月时恢复正常,而我们观察到三个月后CD19 + / CD5 + B细胞扩增以及记忆B细胞持续存在缺陷。慢性移植物抗宿主病对CD8亚群的那些参数没有显着影响,而幼稚的和有能力的CD4亚群则受到很大的影响。但是,慢性移植物抗宿主病最深远的影响是对B细胞亚群,特别是对记忆B人群。晚期严重感染的累积发生率很低(四年时为14%)。使用Cox模型,只有在12个月(P = 0.02)和24个月(P = 0.001)的低B细胞计数与晚期感染的危险相关,特别是如果患者没有发展成慢性移植物抗宿主病。

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