Rho/ROCK/actin signaling regulates membrane androgen receptor induced apoptosis in prostate cancer cells |
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Authors: | Papadopoulou Natalia Charalampopoulos Ioannis Alevizopoulos Konstantinos Gravanis Achille Stournaras Christos |
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Affiliation: | a Department of Biochemistry, University of Crete Medical School, GR-71110 Heraklion, Greece b Pharmacology, University of Crete Medical School, GR-71110 Heraklion, Greece c Medexis-Biotech SA, Kryoneri, Athens, Greece |
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Abstract: | ![]() In this study we describe a novel Rho small GTPase dependent pathway that elicits apoptotic responses controlled by actin reorganization in hormone-sensitive LNCaP- and hormone insensitive DU145-prostate cancer cells stimulated with membrane androgen receptor selective agonists. Using an albumin-conjugated steroid, testosterone-BSA, we now show significant induction of actin polymerization and apoptosis that can be reversed by actin disrupting agents in both cell lines. Testosterone-BSA triggered RhoA/B and Cdc42 activation in DU145 cells followed by stimulation of downstream effectors ROCK, LIMK2 and ADF/destrin. Furthermore, dominant-negative RhoA, RhoB or Cdc42 mutants or pharmacological inhibitors of ROCK inhibited both actin organization and apoptosis in DU145 cells. Activation of RhoA/B and ROCK was also implicated in membrane androgen receptor-dependent actin polymerization and apoptosis in LNCaP cells. Our findings suggest that Rho small GTPases are major membrane androgen receptor effectors controlling actin reorganization and apoptosis in prostate cancer cells. |
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Keywords: | mAR, membrane androgen receptors iAR, intracellular androgen receptors G-actin, globular actin F-actin, filamentous actin FAK, focal adhesion kinase PI-3K, phosphatidylinositol-3 kinase ROCK, Rho-associated coiled-coil-containing protein kinase ADF, actin depolymerizing factor |
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