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Evolving hematopoietic stem cell transplantation strategies in severe aplastic anemia

机译:严重再生障碍性贫血中不断发展的造血干细胞移植策略

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Purpose of reviewSignificant improvements in unrelated donor hematopoietic stem cell transplantation (HSCT) in recent years have solidified its therapeutic role in severe aplastic anemia (SAA) and led to the evolution of treatment algorithms, particularly for children.Recent findingsAdvances in understanding the genetics of inherited bone marrow failure syndromes (IBMFS) have allowed more confidence in accurately diagnosing SAA and avoiding treatments that could be dangerous and ineffective in individuals with IBMFS, which can be diagnosed in 10-20% of children presenting with a picture of SAA. Additionally long-term survival after matched sibling donor and matched unrelated donor HSCT now exceed 90% in children. Late effects after HSCT for SAA are minimal with current strategies, and compare favorably to late effects after upfront immunosuppressive therapy, except for patients with chronic graft versus host disease.SummaryCareful assessment for signs or symptoms of IBMFS, along with genetic screening for these disorders, is of major importance. Matched sibling donor HSCT is already considered the standard of care for upfront therapy and some groups are evaluating matched unrelated donor HSCT as primary therapy. Ongoing studies will continue to challenge treatment algorithms and may lead to an even more expanded role for HSCT in SAA.
机译:综述的目的近年来,无关的供体造血干细胞移植(HSCT)的显着改善已巩固了其在严重再生障碍性贫血(SAA)中的治疗作用,并导致了治疗算法的发展,特别是针对儿童的研究结果。骨髓衰竭综合征(IBMFS)使人们更有信心准确诊断SAA,并避免对IBMFS患者进行危险和无效的治疗,在有SAA图像的10-20%的儿童中可以诊断出这种病。此外,在同等的同胞供体和相配的无关供体HSCT之后,儿童的长期存活率现已超过90%。 HSCT对SAA的晚期影响在目前的策略下是最小的,并且与前期免疫抑制治疗后的晚期影响相比是有利的,除了慢性移植物抗宿主病患者外。总结对IBMFS的体征或症状进行仔细的评估,以及对这些疾病的基因筛查,非常重要。匹配的同胞供体HSCT已被视为前期治疗的标准治疗方法,一些小组正在评估相匹配的无关供体HSCT作为主要疗法。正在进行的研究将继续挑战治疗算法,并可能导致HSCT在SAA中的作用进一步扩大。

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