Decreased Expression in Gastric Cancer and Its Clinical Significance Using VIKOR Method

T. Sri Ranjani, C. Ramadevi
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Abstract

Many cancer-related mortalities are caused by tumour invasion and metastases, which are crucial steps in developing the malignant tumour phenotype. The most significant predictive factor at detection is now the diagnostic stage, depending on the DNM grading system, and the underlying basis behind the development and spread of bladder cancer is still unknown. Hence, additional research on the diagnostic factors linked to the spread and metastasis of stomach cancer would be useful. The production of FENDRR in gastrointestinal cancer cell lines and tissues was compared to that of normal mucosal cells and nearby non-tumour organs using real-time amplicon chain reaction (PCR). The pharmacological effect of FENDRR on gastrointestinal cancer cells was examined using cell viability assays, wound healing tests, and in vitro and in vivo invasive and migration experiments. To evaluate fibronectin1 mRNA and antigen translation, three methods were used: real-time PCR, western blot, and microscopy. Methodology: Antibody, Visualizing, Dilution, Fixative. Assessment options: CD4, CD1a, Q-Bend 10, CD31, Ki67, Tissue transglutaminase. From the end based on Q-Bend 10, the results showed that it received the highest rank, whereas CD4 had the lowest rank. The value of the dataset for decreased expression in the VIKOR method shows that Q-Bend 10 results in the top ranking.
用VIKOR法检测胃癌组织中表达的降低及其临床意义
许多癌症相关的死亡是由肿瘤侵袭和转移引起的,这是恶性肿瘤表型发展的关键步骤。检测时最重要的预测因素现在是诊断阶段,取决于DNM分级系统,膀胱癌发展和扩散背后的潜在基础仍然未知。因此,进一步研究与胃癌扩散和转移有关的诊断因素将是有用的。采用实时扩增链反应(real-time amplicon chain reaction, PCR)技术将胃肠道癌细胞系和组织中FENDRR的产生与正常粘膜细胞和附近非肿瘤器官的产生进行比较。通过细胞活力测定、伤口愈合试验、体外和体内侵袭和迁移实验,研究了FENDRR对胃肠道癌细胞的药理作用。为了评估纤维连接蛋白1 mRNA和抗原翻译,使用了三种方法:实时荧光定量PCR、western blot和显微镜。方法:抗体,可视化,稀释,固定。评估选项:CD4, CD1a, Q-Bend 10, CD31, Ki67,组织转谷氨酰胺酶。从最后基于Q-Bend 10的结果来看,其排名最高,而CD4排名最低。在VIKOR方法中减少表达的数据集的值表明Q-Bend 10在排名中名列前茅。
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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