Harada Hironori, Harada Yuka
Department of Hematology, Juntendo University School of Medicine, Tokyo, Japan.
Cancer Sci. 2015 Apr;106(4):329-36. doi: 10.1111/cas.12614. Epub 2015 Feb 25.
Myelodysplastic syndromes (MDS) are defined as stem cell disorders caused by various gene abnormalities. Recent analysis using next-generation sequencing has provided great advances in identifying relationships between gene mutations and clinical phenotypes of MDS. Gene mutations affecting RNA splicing machinery, DNA methylation, histone modifications, transcription factors, signal transduction proteins and components of the cohesion complex participate in the pathogenesis and progression of MDS. Mutations in RNA splicing and DNA methylation occur early and are considered "founding mutations", whereas others that occur later are regarded as "subclonal mutations". RUNX1 mutations are more likely to subclonal; however, they apparently play a pivotal role in familial MDS. These genetic findings may lead to future therapies for MDS.
骨髓增生异常综合征(MDS)被定义为由各种基因异常引起的干细胞疾病。最近使用下一代测序进行的分析在确定MDS基因突变与临床表型之间的关系方面取得了巨大进展。影响RNA剪接机制、DNA甲基化、组蛋白修饰、转录因子、信号转导蛋白和黏连复合体成分的基因突变参与了MDS的发病机制和进展。RNA剪接和DNA甲基化中的突变发生较早,被认为是“起始突变”,而后来发生的其他突变则被视为“亚克隆突变”。RUNX1突变更可能是亚克隆性的;然而,它们显然在家族性MDS中起关键作用。这些遗传学发现可能会带来未来治疗MDS的方法。
