Human bladder cancer invasion model using rat bladder in vitro and its use to test mechanisms and therapeutic inhibitors of invasion

被引:0
|
作者
C Fujiyama
A Jones
S Fuggle
R Bicknell
D Cranston
A L Harris
机构
[1] Molecular Oncology Unit,Department of Urology
[2] ICRF,Nuffield Department of Surgery
[3] Institute of Molecular Medicine,undefined
[4] John Radcliffe Hospital,undefined
[5] Churchill Hospital,undefined
[6] University of Oxford,undefined
[7] John Radcliffe Hospita,undefined
来源
British Journal of Cancer | 2001年 / 84卷
关键词
invasion; in vitro assay; bladder cancer; suramin; N-acetylcysteine;
D O I
暂无
中图分类号
学科分类号
摘要
As well as being a passive support, the extracellular matrix also regulates key biological processes such as invasion, differentiation and angiogenesis. We have therefore developed an in vitro model of bladder cancer invasion using de-epithelialized rat bladder to allow for tumour cell–extracellular matrix interactions. Onto this we have seeded a panel of human bladder cancer cell lines (RT4, RT112, 253J and EJ28 (T24)) representing progression from well to poorly differentiated phenotypes and used as models of superficial to invasive bladder cancer. The better differentiated cell lines RT4 and RT112 reproducibly grew as stratified epithelium, whereas poorly differentiated EJ28 cells invaded across a broad front. Invasion was not simply related to proliferation rate, measured either as doubling time on plastic (non-invasive 253J and invasive EJ28 having the same doubling time) or by Ki-67 proliferation index within the model. We used the model to test the ability of 4 compounds that interfere with tumour cell–extracellular matrix interactions (suramin, N-acetylcysteine and the urokinase plasminogen activator pathway antagonists Å5 compound and monoclonal antibody Mab 3936) to inhibit invasion. At non-toxic concentrations, all significantly inhibited invasion (P< 0.05), although to varying degrees, suramin and Å5 almost completely and N-acetylcysteine the least. In conclusion, this model shows the urokinase system is important for bladder invasion and can be used to investigate other mechanisms of bladder cancer invasion and also for the testing of intravesical drugs. © 2001 Cancer Research Campaign
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页码:558 / 564
页数:6
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