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Accumulation of genomic alterations in 2p16 9q33.1 and 19p13 in lung tumours of asbestos‐exposed patients

机译:石棉接触患者肺肿瘤中2p16、9q33.1和19p13基因组改变的积累

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摘要

We have previously demonstrated an association between genomic alterations in 19p13, 2p16, and 9q33.1 and asbestos exposure in patients' lung tumours. This study detected allelic imbalance (AI) in these regions in asbestos‐exposed lung cancer (LC) patients' histologically normal pulmonary epithelium. We extended the analyses of tumour tissue to cover a large LC patient cohort and studied DNA copy number alteration (CNA) and AI in 19p13, 2p16, and 9q33.1 for the first time in combination. We found both CNA and AI in ≥2/3 of the regions to be significantly and dose‐dependently (P < 0.001) associated with pulmonary asbestos fibre count. Twenty percent of the exposed patients' LC showed CNA in ≥2/3 of the regions, whereas none of the non‐exposed patients' LC showed CNA in more than one region. AI was evident in 89% of the exposed and in only 26% of the non‐exposed patients' LC. The genomic alterations in 19p13, 2p16, and 9q33.1 in compilation identified asbestos‐exposed patients' lung tumours better than each of the regions alone. These alterations form the basis for the development of a combinatorial molecular assay that could be used to identify asbestos‐related LC.
机译:先前我们已经证明19p13、2p16和9q33.1的基因组改变与患者肺肿瘤中的石棉暴露之间存在关联。这项研究在石棉暴露的肺癌(LC)患者的组织学正常的肺上皮细胞中,发现了这些区域的等位基因失衡(AI)。我们扩展了对肿瘤组织的分析,以涵盖一个大型LC患者队列,并首次组合研究了19p13、2p16和9q33.1中的DNA拷贝数改变(CNA)和AI。我们发现≥2/ 3的区域中的CNA和AI与肺石棉纤维计数显着相关且呈剂量依赖性(P <0.001)。暴露患者的LC中有20%的区域显示≥2/ 3的CNA,而未暴露患者的LC中的一个以上区域均未显示CNA。在89%的接触者和非接触者的LC中,AI很明显。在编辑中的19p13、2p16和9q33.1中的基因组改变确定了接触石棉的患者的肺肿瘤比单独的每个区域更好。这些改变构成了开发可用于鉴定石棉相关LC的组合分子分析的基础。

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