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Immune recovery and immunotherapy after stem cell transplantation in children.

机译:儿童干细胞移植后的免疫恢复和免疫治疗。

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Careful longitudinal studies of the lymphoid cell recovery after stem cell transplantation with other than HLA-identical sibling donors illustrated the prolonged T- and B-cellular immunodeficiency post-SCT, whereas NK-cell recovery was fast. Only low numbers of CD45RO memory T-cells, with a restricted TCR-repertoire, are present in the first 6 months post-SCT. The consequence is an increased risk of viral infections and possibly of leukemia relapse. The latter complication can be prevented by enhancing the anti-leukemic immune reactivity shortly after SCT. Different technical approaches were presented, the majority of them still being in the pre-clinical phase. NK-cell reactivity based on KIR-epitope mismatches between donor and recipient are promising for AML- and CML-, not for ALL-patients. The ALL-blasts may be killed by an antibody-dependent cellular cytotoxicity, using anti-CD19 antibodies, as was shown to be effective in vitro. Also the generation of leukemia-specific CTL's, making use of differences in minor histocompatibility antigens between donor and recipient, is now operational and may be a highly effective approach in a number of leukemic graft recipients.
机译:对与非HLA同胞供体的干细胞移植后的淋巴样细胞恢复进行仔细的纵向研究表明,SCT后T细胞和B细胞免疫缺陷延长,而NK细胞恢复快。在SCT之后的前6个月中,仅有少量的CD45RO记忆T细胞,且TCR记忆库有限。结果是增加了病毒感染和白血病复发的风险。后者的并发症可以通过在SCT后不久增强抗白血病免疫反应性来预防。提出了不同的技术方法,其中大多数仍处于临床前阶段。基于供体和受体之间KIR-表位不匹配的NK细胞反应性有望用于AML和CML,而非ALL患者。如证明在体外有效,可以使用抗CD19抗体通过抗体依赖性细胞的细胞毒性杀死ALL胚细胞。利用供体和受体之间较小的组织相容性抗原的差异,白血病特异性CTL的产生现在也可以操作,并且在许多白血病移植受体中可能是一种非常有效的方法。

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