Figueroa Maria E, Wouters Bas J, Skrabanek Lucy, Glass Jacob, Li Yushan, Erpelinck-Verschueren Claudia A J, Langerak Anton W, Löwenberg Bob, Fazzari Melissa, Greally John M, Valk Peter J M, Melnick Ari, Delwel Ruud
Department of Medicine (Hematology Oncology Division), Weill Cornell Medical College, New York, NY 10021, USA.
Blood. 2009 Mar 19;113(12):2795-804. doi: 10.1182/blood-2008-08-172387. Epub 2009 Jan 23.
Acute myeloid leukemia is a heterogeneous disease from the molecular and biologic standpoints, and even patients with a specific gene expression profile may present clinical and molecular heterogeneity. We studied the epigenetic profiles of a cohort of patients who shared a common gene expression profile but differed in that only half of them harbored mutations of the CEBPA locus, whereas the rest presented with silencing of this gene and coexpression of certain T-cell markers. DNA methylation studies revealed that these 2 groups of patients could be readily segregated in an unsupervised fashion based on their DNA methylation profiles alone. Furthermore, CEBPA silencing was associated with the presence of an aberrant DNA hypermethylation signature, which was not present in the CEBPA mutant group. This aberrant hypermethylation occurred more frequently at sites within CpG islands. CEBPA-silenced leukemias also displayed marked hypermethylation compared with normal CD34(+) hematopoietic cells, whereas CEBPA mutant cases showed only mild changes in DNA methylation compared with these normal progenitors. Biologically, CEBPA-silenced leukemias presented with a decreased response to myeloid growth factors in vitro.
从分子和生物学角度来看,急性髓系白血病是一种异质性疾病,即使具有特定基因表达谱的患者也可能存在临床和分子异质性。我们研究了一组具有共同基因表达谱的患者的表观遗传学特征,但不同的是,其中只有一半患者存在CEBPA基因座突变,而其余患者则表现为该基因沉默以及某些T细胞标志物的共表达。DNA甲基化研究表明,仅根据DNA甲基化谱,这两组患者就可以很容易地以无监督方式区分开来。此外,CEBPA基因沉默与异常的DNA高甲基化特征有关,而CEBPA突变组中不存在这种特征。这种异常的高甲基化在CpG岛内的位点更频繁地发生。与正常CD34(+)造血细胞相比,CEBPA沉默的白血病也表现出明显的高甲基化,而与这些正常祖细胞相比,CEBPA突变病例的DNA甲基化仅表现出轻微变化。从生物学角度来看,CEBPA沉默的白血病在体外对髓系生长因子的反应降低。
