J Clin Invest. 2014 Mar;124(3):1158-67. doi: 10.1172/JCI71264.
Acute myeloid leukemia (AML) is characterized by disruption of HSC and progenitor cell differentiation. Frequently, AML is associated with mutations in genes encoding epigenetic modifiers. We hypothesized that analysis of alterations in DNA methylation patterns during healthy HSC commitment and differentiation would yield epigenetic signatures that could be used to identify stage-specific prognostic subgroups of AML. We performed a nano HpaII-tiny-fragment-enrichment-by-ligation-mediated-PCR (nanoHELP) assay to compare genome-wide cytosine methylation profiles between highly purified human long-term HSC, short-term HSC, common myeloid progenitors, and megakaryocyte-erythrocyte progenitors. We observed that the most striking epigenetic changes occurred during the commitment of short-term HSC to common myeloid progenitors and these alterations were predominantly characterized by loss of methylation. We developed a metric of the HSC commitment–associated methylation pattern that proved to be highly prognostic of overall survival in 3 independent large AML patient cohorts, regardless of patient treatment and epigenetic mutations. Application of the epigenetic signature metric for AML prognosis was superior to evaluation of commitment-based gene expression signatures. Together, our data define a stem cell commitment–associated methylome that is independently prognostic of poorer overall survival in AML.
急性髓系白血病(AML)的特征是造血干细胞(HSC)和祖细胞分化紊乱。通常,AML 与编码表观遗传修饰物的基因突变有关。我们假设,在健康的 HSC 定向分化和分化过程中,对 DNA 甲基化模式的改变进行分析,可能会产生可用于识别 AML 特定预后亚组的表观遗传特征。我们进行了纳米 HpaII-微小片段富集连接介导-PCR(nanoHELP)检测,以比较高度纯化的人类长期 HSC、短期 HSC、共同髓系祖细胞和巨核细胞-红细胞祖细胞之间的全基因组胞嘧啶甲基化谱。我们观察到,最显著的表观遗传变化发生在短期 HSC 向共同髓系祖细胞的定向分化过程中,这些改变主要表现为甲基化缺失。我们开发了一种衡量 HSC 定向分化相关甲基化模式的指标,该指标在 3 个独立的大型 AML 患者队列中,无论患者治疗和表观遗传突变如何,均证明对总生存具有高度预后价值。AML 预后的表观遗传特征指标的应用优于基于定向分化的基因表达特征的评估。综上所述,我们的数据定义了一个与干细胞定向分化相关的甲基组,该甲基组独立地预示 AML 总生存较差。
