Androgen-induced cell migration: role of androgen receptor/filamin A association.

"\"Androgen receptor (AR) controls male morphogenesis, gametogenesis and prostate growth as well as development of prostate cancer. These findings support a role for AR in cell migration and invasiveness. However, the molecular mechanism involved in AR-mediated cell migration still remains elusive.. . Methodology\\\/Principal Findings. Mouse embryo NIH3T3 fibroblasts and highly metastatic human fibrosarcoma HT1080 cells harbor low levels of transcriptionally incompetent AR. We now report that, through extra nuclear action, AR triggers migration of both cell types upon stimulation with physiological concentrations of the androgen R1881. We analyzed the initial events leading to androgen-induced cell migration and observed that challenging NIH3T3 cells with 10 nM R1881 rapidly induces interaction of AR with filamin A (FlnA) at cytoskeleton. AR\\\/FlnA complex recruits integrin beta 1, thus activating its dependent cascade. Silencing of AR, FlnA and integrin beta 1 shows that this ternary complex controls focal adhesion kinase (FAK), paxillin and Rac, thereby driving cell migration. FAK-null fibroblasts migrate poorly and Rac inhibition by EHT impairs motility of androgen-treated NIH3T3 cells. Interestingly, FAK and Rac activation by androgens are independent of each other. Findings in human fibrosarcoma HT1080 cells strengthen the role of Rac in androgen signaling. The Rac inhibitor significantly impairs androgen-induced migration in these cells. A mutant AR, deleted of the sequence interacting with FlnA, fails to mediate FAK activation and paxillin tyrosine phosphorylation in androgen-stimulated cells, further reinforcing the role of AR\\\/FlnA interaction in androgen-mediated motility.. . Conclusions\\\/Significance. The present report, for the first time, indicates that the extra nuclear AR\\\/FlnA\\\/integrin beta 1 complex is the key by which androgen activates signaling leading to cell migration. Assembly of this ternary complex may control organ development and prostate cancer metastasis.\""

"\"Il recettore degli androgeni controlla la morfogenesi, la gametogenesi nonché la crescita e lo sviluppo della ghiandola prostatica. Esso è implicato nella progressione del tumore prostatico. Tali evidenze suggeriscono che il recettore degli androgeni controlla la migrazione cellulare. I meccanismi molecolari con cui avviene tale controllo sono ancora oggi dibattuti.. Il manoscritto dimostra che il classico recettore degli androgeni espresso in cellule mesenchimali, normali o trasformate, interagisce nel compartimento extranucleare con la filmina A e che l'aggiunta di androgeni stabilizza tale legame ed induce l'assemblaggio di un complesso ternario formato da AR\\\/filamina A ed integrina beta 1. Questo complesso da un lato attiva Rac, modificando così' la velocità di migrazione delle cellule, dall'altro induce l'attivazione della chinasi FAK, modulando in tal modo l'adesione cellulare. Il manoscritto descrive per la prima volta il meccanismo molecolare con gli androgeni promuovono la migrazione e l'invalidità di cellule bersaglio attraverso l'attivazione di vie rapide, non genomiche.\""