头颈癌的转录组学和表观基因组学:可用的知识库和分子特征。

Cancers of the head & neck Pub Date : 2020-01-21 eCollection Date: 2020-01-01 DOI:10.1186/s41199-020-0047-y
Mara S Serafini, Laura Lopez-Perez, Giuseppe Fico, Lisa Licitra, Loris De Cecco, Carlo Resteghini
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引用次数: 23

摘要

多年来,头颈部鳞状细胞癌(HNSCC)一直被认为是一个单一的实体。然而,在过去的几十年里,HNSCC的复杂性和异质性已经得到了认识。与此同时,高通量组学技术可以描绘更大范围的癌症分子的行为和特征,并且已经开发了大量基于网络的组学工具和信息库数据库。本综述的目的是对HNSCC的生物学、预后和预测分子特征进行综述。为了将所选数据上下文化,我们的文献调查包括对组学数据存储库和用于数据分析的网络工具的主要特征的简短总结。我们分析的时间框架是固定的,包括2015年1月至2019年1月之间发表的论文。从评估的1000多篇论文中,选择了61篇组学研究:33篇研究mRNA特征,11篇和13篇与miRNA和其他非编码rna特征相关,4篇分析DNA甲基化特征。超过一半的识别特征(36个)具有预后价值,但只有10个研究选择了特定的解剖亚部位(8个口腔,1个口咽和1个口腔和口咽)。值得注意的是,尽管许多研究纳入的样本量有限,但约有一半的检索研究报告了独立数据集的外部验证,加强了所获得数据的相关性。最后,我们强调了三个基因表达特征的开发和利用,它们对预后/治疗反应预测的临床影响可能很高。基于对HNSCC组学相关文献的概述,我们确定了一些局限性和优势。主要的限制是与DNA甲基化和非编码RNA (miRNA, lncRNA和pirna)相关的签名数量较少,以及在500多个HNSCC(即TCGA)上具有多个组学的单个数据集的可用性。主要优势依赖于通过荟萃分析方法整合多个数据集,以及在同一队列患者中获得的组学数据之间的日益整合。此外,基于人工智能和信息分析的新方法有望在未来出现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Transcriptomics and Epigenomics in head and neck cancer: available repositories and molecular signatures.

For many years, head and neck squamous cell carcinoma (HNSCC) has been considered as a single entity. However, in the last decades HNSCC complexity and heterogeneity have been recognized. In parallel, high-throughput omics techniques had allowed picturing a larger spectrum of the behavior and characteristics of molecules in cancer and a large set of omics web-based tools and informative repository databases have been developed. The objective of the present review is to provide an overview on biological, prognostic and predictive molecular signatures in HNSCC. To contextualize the selected data, our literature survey includes a short summary of the main characteristics of omics data repositories and web-tools for data analyses. The timeframe of our analysis was fixed, encompassing papers published between January 2015 and January 2019. From more than 1000 papers evaluated, 61 omics studies were selected: 33 investigating mRNA signatures, 11 and 13 related to miRNA and other non-coding-RNA signatures and 4 analyzing DNA methylation signatures. More than half of identified signatures (36) had a prognostic value but only in 10 studies selection of a specific anatomical sub-site (8 oral cavity, 1 oropharynx and 1 both oral cavity and oropharynx) was performed. Noteworthy, although the sample size included in many studies was limited, about one-half of the retrieved studies reported an external validation on independent dataset(s), strengthening the relevance of the obtained data. Finally, we highlighted the development and exploitation of three gene-expression signatures, whose clinical impact on prognosis/prediction of treatment response could be high. Based on this overview on omics-related literature in HNSCC, we identified some limits and strengths. The major limits are represented by the low number of signatures associated to DNA methylation and to non-coding RNA (miRNA, lncRNA and piRNAs) and the availability of a single dataset with multiple omics on more than 500 HNSCC (i.e. TCGA). The major strengths rely on the integration of multiple datasets through meta-analysis approaches and on the growing integration among omics data obtained on the same cohort of patients. Moreover, new approaches based on artificial intelligence and informatic analyses are expected to be available in the next future.

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