Suppression of EGF-R signaling reduces the incidence of prostate cancer metastasis in nude mice

doi:10.1677/erc.1.01100

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Suppression of EGF-R signaling reduces the incidence of prostate cancer metastasis in nude mice

Adriano Angelucci¹, Giovanni Luca Gravina¹, Nadia Rucci², Danilo Millimaggi², Claudio Festuccia², Paola Muzi², Anna Teti², Carlo Vicentini¹ and Mauro Bologna³

¹ Departments of Surgery,
² Experimental Medicine and
³ Basic and Applied Biology, University of L’Aquila via Vetoio, Coppito 2, 67100 L’Aquila, Italy

(Requests for offprints should be addressed to A Angelucci; Email: adriano.angelucci{at}gmail.com)

The activation of epidermal growth factor receptor (EGF-R) playsa key role in the promotion of proliferation and invasion inprostatic carcinoma (PCa). Gefitinib (Iressa; ZD1839), an orallyactive EGF-R tyrosine kinase inhibitor, has shown an importantanti-proliferative activity in tumors expressing EGF-R bothin vitro and in vivo. Our aim was to elucidate the role of gefitinibin the modulation of the metastatic spread of PCa cells. Thetherapeutic role of gefitinib was investigated by evaluatingthe proliferative and invasive ability of the PCa cell linePC3 and of its high metastatic sub-line, PCb2, by in vitro assaysand intracardiac injection in nude mice. The inhibitory effectof gefitinib was tested in vivo by injecting PCa cells subcutaneouslyor in the left ventricle of nude mice and by administratingdaily 150 mg/kg of gefitinib. While xenograft growth was equallyreduced in all PCa lines (about 50%), the bone metastasis formationwas inhibited especially for the high metastatic PCb2 sub-line(81%) in comparison to PC3 cells (47%). The comparative in vitroanalysis among PCa cell lines showed that PCb2 cells were moresensitive to the inhibitory effect of gefitinib in their invasiveability compared to parental PC3 cells but not in their proliferationrate. Moreover, PCb2 cells demonstrated an increased invasiveability in vitro in response to bone stromal cell conditionedmedium (BCM). The simultaneous presence of 0.1 ng/ml gefitinibwas sufficient to reduce the number of invaded cells in thepresence of both EGF and BCM. The molecular characterizationof the highly aggressive PCa sub-lines demonstrated that thisphenomenon was associated with an increment in uPA/uPAR axisbut not in EGF-R expression. In conclusion, our data suggestthat the use of gefitinib as a therapeutic agent may be indicatedin the control of PCa spreading to bone.

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