Amplification of the urokinase gene and the sensitivity of prostate cancer cells to urokinase inhibitors
OBJECTIVES To evaluate the frequency of the urokinase‐type plasminogen activator (uPA) gene amplification and the sensitivity of prostate cancer cells to uPA inhibition, as we previously found one hormone‐refractory prostate tumour with high‐level amplification of the uPA (alias PLAU) gene, and also...
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Veröffentlicht in: | BJU international 2006-02, Vol.97 (2), p.404-409 |
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Sprache: | eng |
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Zusammenfassung: | OBJECTIVES
To evaluate the frequency of the urokinase‐type plasminogen activator (uPA) gene amplification and the sensitivity of prostate cancer cells to uPA inhibition, as we previously found one hormone‐refractory prostate tumour with high‐level amplification of the uPA (alias PLAU) gene, and also showed that a uPA inhibitor, amiloride, can effectively reduce the invasion potential of the PC‐3 prostate cancer cell line.
MATERIALS AND METHODS
Sixty‐three locally recurrent hormone‐refractory tumours and 78 hormone‐refractory metastases from 29 patients who died from prostate cancer were analysed for uPA gene‐copy number using fluorescence in situ hybridization. The Matrigel invasion assay was used to study the influence of uPA inhibitors on the invasive potential of prostate cancer cell lines.
RESULTS
Of the locally recurrent hormone‐refractory tumours, 21% had an increased copy number of uPA, but no high‐level amplifications were found; 31% of the metastases had increased copy number and one high‐level amplification of the uPA. Matrigel invasion assays with two specific uPA inhibitors, B428 and p‐aminobenzamidine, showed that invasion of a prostate cancer cell line containing uPA gene amplification was inhibited by these small‐molecule uPA inhibitors, while invasion of prostate cell lines without uPA gene amplification were not.
CONCLUSION
These results suggest that selective inhibition of the uPA pathway in individuals whose tumours contain uPA gene amplification may provide therapeutic benefit. |
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ISSN: | 1464-4096 1464-410X |
DOI: | 10.1111/j.1464-410X.2005.05912.x |