Abstract

Human bladder cancer tumors have been shown to contain a subpopulation of cells with stem-like characteristics that may trigger tumor growth, recurrence, and metastasis. These cells, known as tumor-initiating cells (TICs), would be effective diagnostic tools and valuable therapeutic targets. Here, we report the isolation of TICs from seven bladder cancer cell lines and show that TICs from different sources vary on their ability to form tumorspheres in vitro and generate xenografts in vivo, which suggest they are remarkably heterogeneous. We used the Affymetrix PrimeView™ Human Gene Expression Array to analyze gene expression profiles of bladder TICs, which may help understand their tumorigenic capacities and develop novel treatments specifically targeted toward these cells. We then constructed a transcription factor-gene regulatory network that includes three key transcription factors that are involved in cell survival, differentiation, proliferation, and apoptosis. We validated our findings by analyzing mRNA expression of the key genes in this network in 24 clinical tissues. Our results suggest that this transcription factor-gene regulatory network could be useful in the development of clinical diagnostic tools and therapy approaches for bladder cancer.

Highlights

  • Gene expression profiling and construction of a putative gene regulatory network of bladder cancer tumor-initiating cells www.impactjournals.com/oncotarget/

  • The information of each cell from website of American Type Culture Collection, America.

  • Genes ETS1 EGR1 MYC TFRC RPS25 NDUFB3 PDGFC

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Summary

Introduction

Gene expression profiling and construction of a putative gene regulatory network of bladder cancer tumor-initiating cells www.impactjournals.com/oncotarget/

Results
Conclusion

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