Antineoplastic effect of rapamycin is potentiated by inhibition of IRS-1 signaling in prostate cancer cells xenografts

Oliveira, JC; Souza, KK; Dias, MM; Faria, MC; Ropelle, ER; Flores, MBS; Ueno, M; Velloso, LA; Saad, ST; Saad, MJA; Carvalheira, JBC

Artículos de revistas

Registro en:

Journal Of Cancer Research And Clinical Oncology. Springer, v. 134, n. 8, n. 833, n. 839, 2008.

0171-5216

WOS:000256430100002

10.1007/s00432-008-0359-5

http://www.repositorio.unicamp.br/jspui/handle/REPOSIP/77834

http://www.repositorio.unicamp.br/handle/REPOSIP/77834

http://repositorio.unicamp.br/jspui/handle/REPOSIP/77834

http://repositorioslatinoamericanos.uchile.cl/handle/2250/1267126

Autor

Oliveira, JC

Souza, KK

Dias, MM

Faria, MC

Ropelle, ER

Flores, MBS

Ueno, M

Velloso, LA

Saad, ST

Saad, MJA

Carvalheira, JBC

Institución

Universidade Estadual de Campinas (Brasil)

Resumen

Proper activation of phosphoinositide 3-kinase-Akt pathway is critical for the prevention of tumorigenesis. Recent data have characterized a negative feedback loop, wherein mammalian target of rapamycin (mTOR) blocks additional activation of the Akt/mTOR pathway through inhibition insulin receptor substrate 1 (IRS-1) function. However, the potential of IRS-1 inhibition during rapamycin treatment has not been examined. Herein, we show that IRS-1 antisense oligonucleotide and rapamycin synergistically antagonize the activation of mTOR in vivo and induced tumor suppression, through inhibition of proliferation and induction of apoptosis, in prostate cancer cell xenografts. These data demonstrate that the addition of agents that blocks IRS-1 potentiate the effect of mTOR inhibition in the growth of prostate cancer cell xenografts.

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