Vyas Paresh, Crispino John D
Department of Haematology, MRC Molecular Haematology Unit, Weatherall Institute of Molecular Medicine, John Radcliffe Hospital, University of Oxford, Oxford, UK.
Curr Opin Pediatr. 2007 Feb;19(1):9-14. doi: 10.1097/MOP.0b013e328013e7b2.
Four years ago it was discovered that nearly all cases of transient myeloproliferative disorder and acute megakaryocytic leukemia in children with Down syndrome acquire mutations in the hematopoietic transcription factor gene GATA1. Studies within the past year, described within this review, have provided tremendous insights into the role of GATA1 mutations in these malignancies.
In the past year, our understanding of the molecular and cellular consequences of GATA1 mutations has been greatly enhanced. Most importantly, we have learned that these mutations, which result in the exclusive production of the short GATA1 isoform named GATA1s, have a distinct effect on fetal liver progenitors. In addition, multiple studies have shown that GATA1s can substitute for GATA1 in many aspects of megakaryocytic maturation. Finally, an important clinical study has revealed that GATA1 mutations alone are insufficient for leukemia.
Leukemia in children with Down syndrome requires at least three cooperating events--trisomy 21, a GATA1 mutation, and a third, as yet undefined, genetic alteration. Recent studies have provided tremendous insights into the GATA1 side of the story. Future experiments with human patient samples and mouse models will likely increase our awareness of the role of trisomy 21 in transient myeloproliferative disorder and acute megakaryocytic leukemia.
四年前发现,唐氏综合征患儿的几乎所有暂时性骨髓增殖性疾病和急性巨核细胞白血病病例,其造血转录因子基因GATA1都发生了突变。本综述中描述的过去一年的研究,为GATA1突变在这些恶性肿瘤中的作用提供了深刻见解。
在过去一年中,我们对GATA1突变的分子和细胞后果的理解有了极大提高。最重要的是,我们了解到这些突变导致只产生名为GATA1s的短GATA1异构体,对胎儿肝脏祖细胞有独特影响。此外,多项研究表明,GATA1s在巨核细胞成熟的许多方面可替代GATA1。最后,一项重要的临床研究表明,仅GATA1突变不足以引发白血病。
唐氏综合征患儿白血病至少需要三个协同事件——21三体、GATA1突变以及第三个尚未明确的基因改变。最近的研究对GATA1方面提供了深刻见解。未来对人类患者样本和小鼠模型的实验可能会增强我们对21三体在暂时性骨髓增殖性疾病和急性巨核细胞白血病中作用的认识。
