China Oncology ›› 2015, Vol. 25 ›› Issue (7): 505-510.doi: 10.3969/j.issn.1007-3969.2015.07.003

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The expression changes of cancer-related pathways genes screened by RT-PCR Array in bladder cancer

YANG Ke1, FU Bin1,2, WANG Yibing1, WANG Gongxian1,2, LI Junhua, LIU Rensheng1, QI Xueliang1, HUANG Liang1   

  1. 1. Department of Urology, the First Affiliated Hospital of Nanchang University,
    Nanchang Jiangxi 330006, China; 2. Jiangxi Institute of Urology, Nanchang Jiangxi 330006, China
  • Online:2015-07-30 Published:2015-12-09
  • Contact: FU Bin E-mail: fubinncu@gmail.com

Abstract: Background and purpose: Bladder cancer is the most common urological tumor, and its pathogenesis is still not fully understood. The study was aimed to observe the expressions of key genes in many tumor-associated signaling pathways in normal bladder tissue and bladder carcinoma, and to provide further evidence for the subsequent study of bladder cancer recurrence and metastasis. Methods: Twenty-seven cases of bladder cancer specimens were collected, and normal bladder tissues and bladder cancer tissues were distinguished by frozen section. Then, the expressions of 84 genes of cancer-related signaling pathways in bladder cancer tissues and normal bladder tissues were screened by Cancer Pathway Finder PCR Array produced by QIAGEN company. Results: Compared with the normal bladder tissues, the bladder carcinoma tissues had 8 up-regulated genes and 19 down-regulated genes. In this study, the impact of epithelial- mesenchymal transition (EMT) signaling pathway was selected as a research direction in which the GSC, KRT14, DSP were up-regulated, SNAI2, SNAI3 were down-regulated. Therefore GSC, KRT14, DSP, SNAI2 and SNAI3 were chosen as target genes, and verified by qRT-PCR in many examples. The result showed that the expressions of GSC gene in bladder cancer tissues were up-regulated, but with no statistical significance; KRT14, DSP expressions in bladder cancer were higher than those in normal bladder tissues (P<0.05); SNAI2, SNAI3 expressions in bladder cancer were lower than those in normal bladder tissues (P<0.05), and SNAI3 showed the most obvious expression differences. Conclusion: KRT14, DSP and SNAI3 may play an important role in bladder cancer’s occurrence, development and metastasis.

Key words: RT-PCR Array, Bladder cancer, Pathway