Activation of Rac1 is Closely Related to Androgen-independent Cell Proliferation of Prostate Cancer Cells Both in Vitro and in Vivo

Overview

Journal Mol Endocrinol

Specialties Endocrinology
Molecular Biology

Date 2010 Mar 6

PMID 20203103

Citations 31

Authors

Takashi Kobayashi

Takahiro Inoue

Yosuke Shimizu

Naoki Terada

Atsushi Maeno

Yoichiro Kajita

Toshinari Yamasaki

Tomomi Kamba

Yoshinobu Toda

Yoshiki Mikami

Tomomi Yamada

Toshiyuki Kamoto

Osamu Ogawa

Eijiro Nakamura

Affiliations

Soon will be listed here.

Abstract

We and others previously showed that signaling through cSrc or atypical protein kinase C (aPKC) pathway regulates the proliferation of prostate cancer cells and is associated with their progression to castrate-resistance in vivo. However, the interrelation of these two kinases has been largely unexplored. In the present study, we show that androgen-induced activation of cSrc regulates the activity of aPKC through the small molecular weight G protein Rac1 in androgen-dependent LNCaP cells. Knockdown of cSrc in those cells reduces the phosphorylation of aPKC and the abundance of activated form of Rac1. Additionally, the treatment of those cells with Rac1 inhibitor repressed cell cycle progression at G(1)/S transition. In fact, forced expression of a constitutively active Rac1 mutant in LNCaP cells promoted cell proliferation under androgen-depleted conditions both in vitro and in vivo. Moreover, LNCaP C4-2 and AILNCaP cells, the syngeneic androgen-independent sublines from LNCaP cells, harbored abundant Rac1-GTP. Importantly, the inhibition of Rac1 suppressed cell proliferation and induced apoptotic cell death in all prostate cancer cell lines tested irrespective of their androgen-dependence. In immunohistochemical evaluation of tumor specimens from prostate cancer patients, Rac1 pathway appeared to be activated in the majority of castrate-resistant diseases. Collectively, our present results both in vitro and in vivo highly implicate that Rac1 can be a potential therapeutic target for patients with advanced prostate cancer, especially those with castrate-resistant status.

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