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首页> 外文期刊>Journal of Clinical Oncology >Prognostic significance of, and gene and microRNA expression signatures associated with, CEBPA mutations in cytogenetically normal acute myeloid leukemia with high-risk molecular features: a Cancer and Leukemia Group B Study.
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Prognostic significance of, and gene and microRNA expression signatures associated with, CEBPA mutations in cytogenetically normal acute myeloid leukemia with high-risk molecular features: a Cancer and Leukemia Group B Study.

机译:具有高风险分子特征的细胞遗传学正常急性髓性白血病中CEBPA突变的预后意义以及与基因和microRNA表达相关的特征:癌症和白血病B组研究。

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PURPOSE: To evaluate the prognostic significance of CEBPA mutations in the context of established molecular markers in cytogenetically normal (CN) acute myeloid leukemia (AML) and gain biologic insights into leukemogenesis of the CN-AML molecular high-risk subset (FLT3 internal tandem duplication [ITD] positive and/or NPM1 wild type) that has a significantly higher incidence of CEBPA mutations than the molecular low-risk subset (FLT3-ITD negative and NPM1 mutated). PATIENTS AND METHODS: One hundred seventy-five adults age less than 60 years with untreated primary CN-AML were screened before treatment for CEBPA, FLT3, MLL, WT1, and NPM1 mutations and BAALC and ERG expression levels. Gene and microRNA (miRNA) expression profiles were obtained for the CN-AML molecular high-risk patients. RESULTS: CEBPA mutations predicted better event-free (P = .007), disease-free (P = .014), and overall survival (P < .001) independently of other molecular and clinical prognosticators. Among patients with CEBPA mutations,91% were in the CN-AML molecular high-risk group. Within this group, CEBPA mutations predicted better event-free (P < .001), disease-free (P = .004), and overall survival (P = .009) independently of other molecular and clinical characteristics and were associated with unique gene and miRNA expression profiles. The major features of these profiles were upregulation of genes (eg, GATA1, ZFPM1, EPOR, and GFI1B) and miRNAs (ie, the miR-181 family) involved in erythroid differentiation and downregulation of homeobox genes. CONCLUSION: Pretreatment testing for CEBPA mutations identifies CN-AML patients with different outcomes, particularly in the molecular high-risk group, thus improving molecular risk-based classification of this large cytogenetic subset of AML. The gene and miRNA expression profiling provided insights into leukemogenesis of the CN-AML molecular high-risk group, indicating that CEBPA mutations are associated with partial erythroid differentiation.
机译:目的:在细胞遗传学正常(CN)急性髓细胞性白血病(AML)中建立分子标记的背景下评估CEBPA突变的预后意义,并获得有关CN-AML分子高风险亚群(FLT3内部串联复制)白血病发生的生物学见解[ITD]阳性和/或NPM1野生型)的CEBPA突变发生率比分子低风险子集(FLT3-ITD阴性和NPM1突变)高得多。患者和方法:在未治疗的原发性CN-AML患者中筛选了年龄小于60岁的175位成年人,然后进行CEBPA,FLT3,MLL,WT1和NPM1突变以及BAALC和ERG表达水平的治疗。获得了CN-AML分子高危患者的基因和microRNA(miRNA)表达谱。结果:CEBPA突变预测更好的无事件发生率(P = .007),无疾病发生率(P = .014)和总生存期(P <.001),独立于其他分子和临床预后因素。在具有CEBPA突变的患者中,CN-AML分子高风险组占91%。在这一组中,CEBPA突变预测更好的无事件发生率(P <.001),无疾病发生率(P = .004)和总生存期(P = .009),而与其他分子和临床特征无关,并且与独特的基因相关和miRNA表达谱。这些概况的主要特征是参与红系分化和同源异型盒基因下调的基因(例如GATA1,ZFPM1,EPOR和GFI1B)和miRNA(即miR-181家族)的上调。结论:CEBPA突变的预处理测试可识别出具有不同结局的CN-AML患者,特别是在分子高危人群中,从而改善了这种基于AML的大细胞遗传学亚型的基于分子风险的分类。该基因和miRNA表达谱提供了对CN-AML分子高危人群白血病发生的见解,表明CEBPA突变与部分红系分化有关。

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