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一组转录因子的活性与急性髓系白血病的干细胞程序和临床结果相关。

Activity of a heptad of transcription factors is associated with stem cell programs and clinical outcome in acute myeloid leukemia.

机构信息

Lowy Cancer Research Centre and the Prince of Wales Clinical School, University of New South Wales, Sydney, Australia.

出版信息

Blood. 2013 Mar 21;121(12):2289-300. doi: 10.1182/blood-2012-07-446120. Epub 2013 Jan 17.

Abstract

Aberrant transcriptional programs in combination with abnormal proliferative signaling drive leukemic transformation. These programs operate in normal hematopoiesis where they are involved in hematopoietic stem cell (HSC) proliferation and maintenance. Ets Related Gene (ERG) is a component of normal and leukemic stem cell signatures and high ERG expression is a risk factor for poor prognosis in acute myeloid leukemia (AML). However, mechanisms that underlie ERG expression in AML and how its expression relates to leukemic stemness are unknown. We report that ERG expression in AML is associated with activity of the ERG promoters and +85 stem cell enhancer and a heptad of transcription factors that combinatorially regulate genes in HSCs. Gene expression signatures derived from ERG promoter-stem cell enhancer and heptad activity are associated with clinical outcome when ERG expression alone fails. We also show that the heptad signature is associated with AMLs that lack somatic mutations in NPM1 and confers an adverse prognosis when associated with FLT3 mutations. Taken together, these results suggest that transcriptional regulators cooperate to establish or maintain primitive stem cell-like signatures in leukemic cells and that the underlying pattern of somatic mutations contributes to the development of these signatures and modulate their influence on clinical outcome.

摘要

异常的转录程序与异常的增殖信号共同驱动白血病的转化。这些程序在正常造血中起作用,参与造血干细胞(HSC)的增殖和维持。Ets 相关基因(ERG)是正常和白血病干细胞特征的组成部分,高 ERG 表达是急性髓系白血病(AML)预后不良的危险因素。然而,AML 中 ERG 表达的机制及其与白血病干性的关系尚不清楚。我们报告称,AML 中的 ERG 表达与 ERG 启动子-干细胞增强子的活性以及一组 7 个转录因子有关,这些转录因子组合调控 HSCs 中的基因。当 ERG 表达单独不能预测临床结果时,从 ERG 启动子-干细胞增强子和七联体活性中获得的基因表达特征与临床结果相关。我们还表明,七联体特征与缺乏 NPM1 体细胞突变的 AML 相关,并且在与 FLT3 突变相关时,会带来不良预后。综上所述,这些结果表明转录调节剂合作在白血病细胞中建立或维持原始干细胞样特征,并且潜在的体细胞突变模式有助于这些特征的发展,并调节它们对临床结果的影响。

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