Leukemogenesis in infants and young children with trisomy 21.

IF 2.9 3区 教育学 Q1 EDUCATION, SCIENTIFIC DISCIPLINES Hematology. American Society of Hematology. Education Program Pub Date : 2022-12-09 DOI:10.1182/hematology.2022000395
Irene Roberts
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引用次数: 4

Abstract

Children with Down syndrome (DS) have a greater than 100-fold increased risk of developing acute myeloid leukemia (ML) and an approximately 30-fold increased risk of acute lymphoblastic leukemia (ALL) before their fifth birthday. ML-DS originates in utero and typically presents with a self-limiting, neonatal leukemic syndrome known as transient abnormal myelopoiesis (TAM) that is caused by cooperation between trisomy 21-associated abnormalities of fetal hematopoiesis and somatic N-terminal mutations in the transcription factor GATA1. Around 10% of neonates with DS have clinical signs of TAM, although the frequency of hematologically silent GATA1 mutations in DS neonates is much higher (~25%). While most cases of TAM/silent TAM resolve without treatment within 3 to 4 months, in 10% to 20% of cases transformation to full-blown leukemia occurs within the first 4 years of life when cells harboring GATA1 mutations persist and acquire secondary mutations, most often in cohesin genes. By contrast, DS-ALL, which is almost always B-lineage, presents after the first few months of life and is characterized by a high frequency of rearrangement of the CRLF2 gene (60%), often co-occurring with activating mutations in JAK2 or RAS genes. While treatment of ML-DS achieves long-term survival in approximately 90% of children, the outcome of DS-ALL is inferior to ALL in children without DS. Ongoing studies in primary cells and model systems indicate that the role of trisomy 21 in DS leukemogenesis is complex and cell context dependent but show promise in improving management and the treatment of relapse, in which the outcome of both ML-DS and DS-ALL remains poor.

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21三体婴幼儿白血病的发生。
患有唐氏综合症(DS)的儿童在5岁生日前患急性髓性白血病(ML)的风险增加了100倍以上,患急性淋巴细胞白血病(ALL)的风险增加了约30倍。ML-DS起源于子宫,通常表现为一种自限性新生儿白血病综合征,称为短暂性骨髓增生异常(TAM),由21三体相关的胎儿造血异常和转录因子GATA1的体细胞n端突变共同引起。大约10%的DS新生儿有TAM的临床症状,尽管在DS新生儿中血液学沉默的GATA1突变的频率要高得多(~25%)。虽然大多数TAM/沉默性TAM病例无需治疗即可在3至4个月内消退,但在10%至20%的病例中,当携带GATA1突变的细胞持续存在并获得继发性突变时,会在生命的头4年内转变为全面白血病,最常见的是在黏结蛋白基因中。相比之下,DS-ALL几乎都是b系,在出生后几个月出现,其特征是CRLF2基因重排的频率很高(60%),通常与JAK2或RAS基因的激活突变共同发生。虽然ML-DS的治疗在大约90%的儿童中实现了长期生存,但DS-ALL在没有DS的儿童中的预后不如ALL。正在进行的原代细胞和模型系统研究表明,21三体在DS白血病发生中的作用是复杂的,并且依赖于细胞环境,但在改善管理和治疗复发方面显示出希望,其中ML-DS和DS- all的结果仍然很差。
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来源期刊
Hematology. American Society of Hematology. Education Program
Hematology. American Society of Hematology. Education Program EDUCATION, SCIENTIFIC DISCIPLINES-HEMATOLOGY
CiteScore
4.70
自引率
3.30%
发文量
0
期刊介绍: Hematology, the ASH Education Program, is published annually by the American Society of Hematology (ASH) in one volume per year.
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