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DNA methylation-based biomarkers for early detection of non-small cell lung cancer: an update

机译:基于DNA甲基化的生物标记物可用于非小细胞肺癌的早期检测:最新进展

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摘要

Lung cancer is the number one cancer killer in the United States. This disease is clinically divided into two sub-types, small cell lung cancer, (10–15% of lung cancer cases), and non-small cell lung cancer (NSCLC; 85–90% of cases). Early detection of NSCLC, which is the more common and less aggressive of the two sub-types, has the highest potential for saving lives. As yet, no routine screening method that enables early detection exists, and this is a key factor in the high mortality rate of this disease. Imaging and cytology-based screening strategies have been employed for early detection, and while some are sensitive, none have been demonstrated to reduce lung cancer mortality. However, mortality might be reduced by developing specific molecular markers that can complement imaging techniques. DNA methylation has emerged as a highly promising biomarker and is being actively studied in multiple cancers. The analysis of DNA methylation-based biomarkers is rapidly advancing, and a large number of potential biomarkers have been identified. Here we present a detailed review of the literature, focusing on DNA methylation-based markers developed using primary NSCLC tissue. Viable markers for clinical diagnosis must be detectable in 'remote media' such as blood, sputum, bronchoalveolar lavage, or even exhaled breath condensate. We discuss progress on their detection in such media and the sensitivity and specificity of the molecular marker panels identified to date. Lastly, we look to future advancements that will be made possible with the interrogation of the epigenome.
机译:肺癌是美国排名第一的癌症杀手。该疾病在临床上分为两种亚型:小细胞肺癌(占肺癌病例的10-15%)和非小细胞肺癌(NSCLC;占病例的85-90%)。早期检测NSCLC是两种亚型中较常见且较弱的一种,具有挽救生命的最大潜力。迄今为止,尚无能够早期发现的常规筛查方法,这是该疾病高死亡率的关键因素。基于影像学和细胞学的筛查策略已用于早期检测,尽管有些策略很灵敏,但尚无降低肺癌死亡率的证据。但是,通过开发可以补充成像技术的特定分子标记可以降低死亡率。 DNA甲基化已成为一种很有前途的生物标志物,并且正在多种癌症中进行积极研究。基于DNA甲基化的生物标记物的分析正在迅速推进,并且已经鉴定出大量潜在的生物标记物。在这里,我们介绍文献的详细审查,重点放在使用原发性NSCLC组织开发的基于DNA甲基化的标记物上。用于临床诊断的可行标记物必须在“远程培养基”中可以检测到,例如血液,痰液,支气管肺泡灌洗液,甚至呼出的呼吸道冷凝物。我们讨论了在此类介质中检测它们的进展以及迄今为止确定的分子标记物组的敏感性和特异性。最后,我们期待通过表观基因组的询问将可能实现的未来发展。

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