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Alterations of tumor-related genes do not exactly match the histopathological grade in gastric adenocarcinomas

机译:胃腺癌中与肿瘤相关的基因改变与组织病理学分级不完全匹配

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摘要

AIM: To investigate the diverse characteristics of different pathological gradings of gastric adenocarcinoma (GA) using tumor-related genes.METHODS: GA tissues in different pathological gradings and normal tissues were subjected to tissue arrays. Expressions of 15 major tumor-related genes were detected by RNA in situ hybridization along with 3’ terminal digoxin-labeled anti-sense single stranded oligonucleotide and locked nucleic acid modifying probe within the tissue array. The data obtained were processed by support vector machines by four different feature selection methods to discover the respective critical gene/gene subsets contributing to the GA activities of different pathological gradings.RESULTS: In comparison of poorly differentiated GA with normal tissues, tumor-related gene TP53 plays a key role, although other six tumor-related genes could also achieve the Area Under Curve (AUC) of the receiver operating characteristic independently by more than 80%. Comparing the well differentiated GA with normal tissues, we found that 11 tumor-related genes could independently obtain the AUC by more than 80%, but only the gene subsets, TP53, RB and PTEN, play a key role. Only the gene subsets, Bcl10, UVRAG, APC, Beclin1, NM23, PTEN and RB could distinguish between the poorly differentiated and well differentiated GA. None of a single gene could obtain a valid distinction.CONCLUSION: Different from the traditional point of view, the well differentiated cancer tissues have more alterations of important tumor-related genes than the poorly differentiated cancer tissues.
机译:目的:利用肿瘤相关基因探讨胃腺癌(GA)不同病理学分级的不同特征。方法:对不同病理学分级的GA组织和正常组织进行组织芯片检测。通过RNA原位杂交以及3'末端地高辛标记的反义单链寡核苷酸和锁定的核酸修饰探针在组织阵列中检测到15种主要的肿瘤相关基因的表达。支持向量机通过四种不同的特征选择方法对获得的数据进行处理,以发现有助于不同病理分级的GA活动的各个关键基因/基因亚组。结果:与肿瘤正常组织相比,低分化GA与肿瘤相关基因进行了比较TP53起着关键作用,尽管其他六个与肿瘤相关的基因也可以独立地以超过80%的比例实现接收器工作特性的曲线下面积(AUC)。将分化良好的GA与正常组织进行比较,我们发现11个与肿瘤相关的基因可以独立获得80%以上的AUC,但是只有TP53,RB和PTEN的基因亚群才发挥关键作用。只有基因亚群,Bcl10,UVRAG,APC,Beclin1,NM23,PTEN和RB可以区分低分化和高分化GA。结论:与传统观点不同,高分化癌组织比低分化癌组织具有更多重要的肿瘤相关基因变异。

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