长链非编码rna的5-羟甲基化水平用于非侵袭性癌症诊断前的考虑。

Zhou Zhang, Chang Zeng, Wei Zhang
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引用次数: 2

摘要

以往的研究表明,5-羟甲基胞嘧啶(5hmC)异常修饰与癌症病理生物学有关。利用高度敏感的基于化学标记的5hmC- seal技术对循环无细胞DNA (cfDNA)中的5hmC进行全基因组分析,已被证明具有成为发现癌症生物标志物的强大表观基因组工具的潜力。先前的研究主要集中在cfdna衍生的5hmC-Seal数据中,这些数据汇总在注释良好的基因特征(如基因体)或无偏箱中。Zhou等人最近利用公开的5hmC-Seal数据,提出长链非编码rna (lncRNAs)作为生物标志物发现的另一种分子靶标。考虑到其潜在的临床影响,我们想评论周等人,并提倡更认真地考虑关键问题,如临床信息和技术变量的可用性,特别是在使用公开可用的数据进行二次分析时,以提高数据透明度和可翻译性。
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Considerations before the application of 5-hydroxymethylation levels of long non-coding RNAs for non-invasive cancer diagnosis.

Previous studies have suggested that aberrant 5-hydroxymethylcytosines (5hmC) modifications are related to cancer pathobiology. Genome-wide profiling 5hmC in circulating cell-free DNA (cfDNA) using the highly sensitive chemical labeling-based 5hmC-Seal technique has been demonstrated to have the potential to be a robust epigenomic tool for cancer biomarker discovery. Prior studies have mostly focused on cfDNA-derived 5hmC-Seal data summarized in well-annotated genic features (e.g., gene bodies) or unbiased bins. Zhou et al. recently proposed long non-coding RNAs (lncRNAs) as an alternative molecular target for biomarker discovery using publicly available 5hmC-Seal data. Considering its potential clinical impact, we would like to comment on Zhou et al. and advocate more serious consideration of critical issues such as the availability of clinical information and technical variables, especially when performing secondary analysis using publicly available data, with the aim of improving data transparency and translatability.

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