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首页> 外文期刊>Leukemia >DNA profiling analysis of 100 consecutive de novo acute myeloid leukemia cases reveals patterns of genomic instability that affect all cytogenetic risk groups
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DNA profiling analysis of 100 consecutive de novo acute myeloid leukemia cases reveals patterns of genomic instability that affect all cytogenetic risk groups

机译:连续100例从头进行的急性髓细胞性白血病病例的DNA谱分析分析揭示了影响所有细胞遗传风险组的基因组不稳定模式

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摘要

We have carried out a high-resolution whole genome DNA profiling analysis on 100 bone marrow samples from a consecutive series of de novo acute myeloid leukemia (AML) cases. After discarding copy number changes that are known to be genetic polymorphisms, we found that genomic aberrations (GA) in the form of gains or losses of genetic material were present in 74% of the samples, with a median of 2 GA per case (range 0–35). In addition to the cytogenetically detected aberration, GA were present in cases from all cytogenetic prognostic groups: 79% in the favorable group, 60% in the intermediate group (including 59% of cases with normal karyotype) and 83% in the adverse group. Five aberrant deleted regions were recurrently associated with cases with a highly aberrant genome (e.g., a 1.5Mb deletion at 17q11.2 and a 750kb deletion at 5q31.1). Different degrees of genomic instability showed a statistically significant impact on survival curves, even within the normal karyotype cases. This association was independent of other clinical and genetic parameters. Our study provides, for the first time, a detailed picture of the nature and frequency of DNA copy number aberrations in de novo AML.
机译:我们已经对来自一系列连续的从头急性髓性白血病(AML)病例的100个骨髓样品进行了高分辨率全基因组DNA分析。丢弃已知为遗传多态性的拷贝数变化后,我们发现74%的样本中存在遗传物质得失形式的基因组畸变(GA),每例中位数为2 GA(范围0-35)。除通过细胞遗传学检测到的畸变外,所有细胞遗传学预后组的病例中均存在GA:有利组为79%,中间组为60%(包括核型正常的患者为59%),中间组为83%。不利群体。五个异常缺失区与具有高度异常基因组的病例(例如在17q11.2缺失1.5Mb和在5q31.1缺失750kb)经常相关。即使在正常的核型病例中,不同程度的基因组不稳定性也显示出对存活曲线的统计学显着影响。这种关联独立于其他临床和遗传参数。我们的研究首次提供了从头反洗钱中DNA拷贝数畸变的性质和频率的详细图片。

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