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Prognostically useful gene-expression profiles in acute myeloid leukemia.

机译:在急性髓性白血病中对预后有用的基因表达谱。

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BACKGROUND: In patients with acute myeloid leukemia (AML) a combination of methods must be used to classify the disease, make therapeutic decisions, and determine the prognosis. However, this combined approach provides correct therapeutic and prognostic information in only 50 percent of cases. METHODS: We determined the gene-expression profiles in samples of peripheral blood or bone marrow from 285 patients with AML using Affymetrix U133A GeneChips containing approximately 13,000 unique genes or expression-signature tags. Data analyses were carried out with Omniviz, significance analysis of microarrays, and prediction analysis of microarrays software. Statistical analyses were performed to determine the prognostic significance of cases of AML with specific molecular signatures. RESULTS: Unsupervised cluster analyses identified 16 groups of patients with AML on the basis of molecular signatures. We identified the genes that defined these clusters and determined the minimal numbers of genes needed to identify prognostically important clusters with a high degree of accuracy. The clustering was driven by the presence of chromosomal lesions (e.g., t(8;21), t(15;17), and inv(16)), particular genetic mutations (CEBPA), and abnormal oncogene expression (EVI1). We identified several novel clusters, some consisting of specimens with normal karyotypes. A unique cluster with a distinctive gene-expression signature included cases of AML with a poor treatment outcome. CONCLUSIONS: Gene-expression profiling allows a comprehensive classification of AML that includes previously identified genetically defined subgroups and a novel cluster with an adverse prognosis.
机译:背景:对于患有急性髓性白血病(AML)的患者,必须使用多种方法对疾病进行分类,做出治疗决定并确定预后。但是,这种组合方法仅在50%的病例中提供了正确的治疗和预后信息。方法:我们使用含有大约13,000个独特基因或表达签名标签的Affymetrix U133A GeneChips确定了285例AML患者外周血或骨髓样本中的基因表达谱。使用Omniviz进行数据分析,对微阵列进行显着性分析,并对微阵列软件进行预测分析。进行统计分析以确定具有特定分子特征的AML病例的预后意义。结果:无监督的聚类分析基于分子特征识别了16组AML患者。我们鉴定了定义这些簇的基因,并确定了以高度准确度鉴定对预后重要的簇所需的基因最少数目。聚集是由存在染色体损伤(例如t(8; 21),t(15; 17)和inv(16)),特定的基因突变(CEBPA)和异常的癌基因表达(EVI1)驱动的。我们确定了几个新的类群,其中一些由具有正常核型的标本组成。具有独特的基因表达特征的独特簇包括治疗效果差的AML病例。结论:基因表达谱分析可以对AML进行全面分类,包括先前鉴定的遗传定义的亚组和具有不良预后的新型簇。

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