Preudhomme Claude, Renneville Aline, Bourdon Violaine, Philippe Nathalie, Roche-Lestienne Catherine, Boissel Nicolas, Dhedin Nathalie, André Jean-Marie, Cornillet-Lefebvre Pascale, Baruchel André, Mozziconacci Marie-Joelle, Sobol Hagay
Department of Hematology, Biology and Pathology Center, Centre Hospitalier Régional Universitaire (CHRU) of Lille, Lille, France.
Blood. 2009 May 28;113(22):5583-7. doi: 10.1182/blood-2008-07-168260. Epub 2009 Apr 8.
Familial platelet disorder (FPD), a rare autosomal dominant disorder characterized by quantitative and qualitative platelet abnormalities, is considered as a model of genetic predisposition to acute myeloid leukemia (AML). So far, monoallelic RUNX1 germline mutations have been found in 19 of 20 families with reported FPD, and the analysis of blast cells from only 5 patients at acute leukemia (AL) stage has shown no additional RUNX1 abnormality. Here, we performed RUNX1 analysis at constitutional and somatic levels in 8 persons with FPD who developed AL from 4 independent families. In addition to the germline RUNX1 mutation, we identified a second RUNX1 alteration in 6 AML cases (acquired point mutations in 4 cases and duplication of the altered RUNX1 allele associated with acquired trisomy 21 in 2 other cases). Although haploinsufficiency of RUNX1 causes FPD, our findings suggest that a second genetic event involving RUNX1 is often associated with progression to AML.
家族性血小板疾病(FPD)是一种罕见的常染色体显性疾病,其特征为血小板数量和质量异常,被视为急性髓系白血病(AML)遗传易感性的模型。到目前为止,在已报道的20个FPD家族中的19个家族中发现了单等位基因RUNX1种系突变,并且仅对5例处于急性白血病(AL)阶段患者的原始细胞进行分析,未发现RUNX1有其他异常。在此,我们对来自4个独立家族且发展为AL的8例FPD患者进行了RUNX1基因构成水平和体细胞水平的分析。除了种系RUNX1突变外,我们在6例AML病例中鉴定出了第二个RUNX1改变(4例为获得性点突变,另外2例为与获得性21三体相关的改变的RUNX1等位基因重复)。虽然RUNX1单倍剂量不足会导致FPD,但我们的研究结果表明,涉及RUNX1的第二次遗传事件通常与进展为AML有关。
