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Overview of major molecular alterations during progression from Barrett's esophagus to esophageal adenocarcinoma

机译:Barrett食管进展过程中的主要分子改变概述对食管腺癌

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Esophageal adenocarcinoma (EAC) develops in the sequential transformation of normal epithelium into metaplastic epithelium, called Barrett's esophagus (BE), then to dysplasia, and finally cancer. BE is a common condition in which normal stratified squamous epithelium of the esophagus is replaced with an intestine-like columnar epithelium, and it is the most prominent risk factor for EAC. This review aims to impartially systemize the knowledge from a large number of publications that describe the molecular and biochemical alterations occurring over this progression sequence. In order to provide an unbiased extraction of the knowledge from the literature, a text-mining methodology was used to select genes that are involved in the BE progression, with the top candidate genes found to be TP53, CDKN2A, CTNNB1, CDH1, GPX3, and NOX5. In addition, sample frequencies across analyzed patient cohorts at each stage of disease progression are summarized. All six genes are altered in the majority of EAC patients, and accumulation of alterations correlates well with the sequential progression of BE to cancer, indicating that the textmining method is a valid approach for gene prioritization. This review discusses how, besides being cancer drivers, these genes are functionally interconnected and might collectively be considered a central hub of BE progression.
机译:食管腺癌(EAC)在正常上皮的连续转化中发展到常规上皮,称为Barrett的食道(BE),然后对发育不良,最后癌症。是一种常见的状态,其中食道正常分层鳞状上皮被肠状柱状上皮替换,并且是EAC最突出的危险因素。本综述旨在公平地系统化来自大量出版物的知识,所述出版物描述了在该进展顺序上发生的分子和生化改变。为了提供从文献中的知识的无偏见的提取,使用文本挖掘方法来选择参与进展的基因,发现候选基因是TP53,CDKN2A,CTNNB1,CDH1,GPX3,和nox5。此外,总结了在疾病进展的每个阶段分析的患者群体的样本频率。所有六种基因都在大多数EAC患者中改变,改变的积累随着对癌症的连续进展良好相关,表明Textmining方法是基因优先级的有效方法。本次审查讨论了除癌症司机之外,这些基因在功能上互联,可能集体被认为是进展的中心枢纽。

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