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首页> 外文期刊>Journal of Clinical Oncology >Quantitative DNA methylation analysis identifies a single CpG dinucleotide important for ZAP-70 expression and predictive of prognosis in chronic lymphocytic leukemia
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Quantitative DNA methylation analysis identifies a single CpG dinucleotide important for ZAP-70 expression and predictive of prognosis in chronic lymphocytic leukemia

机译:定量DNA甲基化分析可鉴定出一个单一的CpG二核苷酸,该蛋白对ZAP-70的表达非常重要,并可预测慢性淋巴细胞性白血病的预后

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Purpose: Increased ZAP-70 expression predicts poor prognosis in chronic lymphocytic leukemia (CLL). Current methods for accurately measuring ZAP-70 expression are problematic, preventing widespread application of these tests in clinical decision making. We therefore used comprehensive DNA methylation profiling of the ZAP-70 regulatory region to identify sites important for transcriptional control. Patients and Methods: High-resolution quantitative DNA methylation analysis of the entire ZAP-70 gene regulatory regions was conducted on 247 samples from patients with CLL from four independent clinical studies. Results: Through this comprehensive analysis, we identified a small area in the 5′ regulatory region of ZAP-70 that showed large variability in methylation in CLL samples but was universally methylated in normal B cells. High correlation with mRNA and protein expression, as well as activity in promoter reporter assays, revealed that within this differentially methylated region, a single CpG dinucleotide and neighboring nucleotides are particularly important in ZAP-70 transcriptional regulation. Furthermore, by using clustering approaches, we identified a prognostic role for this site in four independent data sets of patients with CLL using time to treatment, progression-free survival, and overall survival as clinical end points. Conclusion: Comprehensive quantitative DNA methylation analysis of the ZAP-70 gene in CLL identified important regions responsible for transcriptional regulation. In addition, loss of methylation at a specific single CpG dinucleotide in the ZAP-70 5′ regulatory sequence is a highly predictive and reproducible biomarker of poor prognosis in this disease. This work demonstrates the feasibility of using quantitative specific ZAP-70 methylation analysis as a relevant clinically applicable prognostic test in CLL.
机译:目的:增加ZAP-70表达可预测慢性淋巴细胞性白血病(CLL)的预后不良。当前准确测量ZAP-70表达的方法存在问题,从而阻止了这些测试在临床决策中的广泛应用。因此,我们使用了ZAP-70调控区的全面DNA甲基化图谱来鉴定对转录控制重要的位点。患者和方法:对来自四个独立临床研究的CLL患者的247个样品进行了整个ZAP-70基因调控区域的高分辨率定量DNA甲基化分析。结果:通过这项全面的分析,我们在ZAP-70的5'调控区域中发现了一个小区域,该区域在CLL样品中甲基化表现出较大的变异性,但在正常B细胞​​中普遍被甲基化。与mRNA和蛋白质表达以及启动子报告基因测定中的活性高度相关,表明在该差异甲基化区域内,单个CpG二核苷酸和邻近核苷酸在ZAP-70转录调控中特别重要。此外,通过使用聚类方法,我们以治疗时间,无进展生存期和总体生存期为临床终点,在四个独立的CLL患者数据集中确定了该部位的预后作用。结论:CLL中ZAP-70基因的全面定量DNA甲基化分析确定了负责转录调控的重要区域。另外,在ZAP-70 5'调节序列中特定的单个CpG二核苷酸处的甲基化损失是该疾病预后不良的高度可预测和可再现的生物标志物。这项工作证明了使用定量特异性ZAP-70甲基化分析作为CLL中相关的临床适用预后测试的可行性。

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