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胃癌的分子改变,特别涉及早发型亚型。

Molecular alterations in gastric cancer with special reference to the early-onset subtype.

作者信息

Skierucha Małgorzata, Milne Anya Na, Offerhaus G Johan A, Polkowski Wojciech P, Maciejewski Ryszard, Sitarz Robert

机构信息

Małgorzata Skierucha, Ryszard Maciejewski, Robert Sitarz, Department of Human Anatomy, Medical University of Lublin, 20-950 Lublin, Poland.

出版信息

World J Gastroenterol. 2016 Feb 28;22(8):2460-74. doi: 10.3748/wjg.v22.i8.2460.

DOI:10.3748/wjg.v22.i8.2460
PMID:26937134
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4768192/
Abstract

Currently, gastric cancer (GC) is one of the most frequently diagnosed neoplasms, with a global burden of 723000 deaths in 2012. It is the third leading cause of cancer-related death worldwide. There are numerous possible factors that stimulate the pro-carcinogenic activity of important genes. These factors include genetic susceptibility expressed in a single-nucleotide polymorphism, various acquired mutations (chromosomal instability, microsatellite instability, somatic gene mutations, epigenetic alterations) and environmental circumstances (e.g., Helicobcter pylori infection, EBV infection, diet, and smoking). Most of the aforementioned pathways overlap, and authors agree that a clear-cut pathway for GC may not exist. Thus, the categorization of carcinogenic events is complicated. Lately, it has been claimed that research on early-onset gastric carcinoma (EOGC) and hereditary GC may contribute towards unravelling some part of the mystery of the GC molecular pattern because young patients are less exposed to environmental carcinogens and because carcinogenesis in this setting may be more dependent on genetic factors. The comparison of various aspects that differ and coexist in EOGCs and conventional GCs might enable scientists to: distinguish which features in the pathway of gastric carcinogenesis are modifiable, discover specific GC markers and identify a specific target. This review provides a summary of the data published thus far concerning the molecular characteristics of GC and highlights the outstanding features of EOGC.

摘要

目前,胃癌是最常被诊断出的肿瘤之一,2012年全球胃癌死亡病例达723000例。它是全球癌症相关死亡的第三大主要原因。有许多可能的因素会刺激重要基因的致癌活性。这些因素包括单核苷酸多态性所表达的遗传易感性、各种获得性突变(染色体不稳定、微卫星不稳定、体细胞基因突变、表观遗传改变)以及环境因素(如幽门螺杆菌感染、EB病毒感染、饮食和吸烟)。上述大多数途径相互重叠,作者们一致认为可能不存在明确的胃癌致癌途径。因此,致癌事件的分类很复杂。最近,有人声称对早发性胃癌(EOGC)和遗传性胃癌的研究可能有助于揭开胃癌分子模式之谜的一部分,因为年轻患者较少接触环境致癌物,而且在这种情况下致癌作用可能更依赖于遗传因素。比较早发性胃癌和传统胃癌中不同且共存的各个方面,可能使科学家能够:区分胃癌致癌途径中哪些特征是可改变的,发现特定的胃癌标志物并确定特定靶点。本综述总结了迄今为止发表的有关胃癌分子特征的数据,并突出了早发性胃癌的显著特征。

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本文引用的文献

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Individual having a parent with early-onset gastric cancer may need screening at younger age.父母患有早发性胃癌的个体可能需要在更年轻时进行筛查。
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Gastrin May Mediate the Carcinogenic Effect of Helicobacter pylori Infection of the Stomach.胃泌素可能介导幽门螺杆菌胃部感染的致癌作用。
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Is microsatellite instability a prognostic marker in gastric cancer? A systematic review with meta-analysis.微卫星不稳定性是否是胃癌的预后标志物?一项系统评价和荟萃分析。
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Clinicopathological characteristics and chronology of p53 expression in the development of gastric cancer.胃癌发生过程中p53表达的临床病理特征及时间顺序
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