Channing Paller1, Hong Pu2, Diane E Begemann3, Cameron A Wade2, Patrick J Hensley2, Natasha Kyprianou2,3,4. 1. The Johns Hopkins Kimmel Cancer Center and Department of Medicine, Johns Hopkins University, Baltimore, Maryland. 2. Department of Urology, University of Kentucky College of Medicine, Lexington, Kentucky. 3. Department of Toxicology and Cancer Biology, University of Kentucky College of Medicine, Lexington, Kentucky. 4. Department of Molecular and Cellular Biochemistry, University of Kentucky College of Medicine, Lexington, Kentucky.
Abstract
BACKGROUND: Prostate cancer progression is navigated by the androgen receptor (AR) and transforming-growth factor-β (TGF-β) signaling. We previously demonstrated that aberrant TGF-β signaling accelerates prostate tumor progression in a transgenic mouse model of prostate cancer via effects on epithelial-mesenchymal transition (EMT), driving castration-resistant prostate cancer (CRPC). METHODS: This study examined the antitumor effect of the combination of TGF-β receptor I (TβRI) inhibitor, galunisertib, and FDA-approved antiandrogen enzalutamide, in our pre-clinical model. Age-matched genotypically characterized DNTGFβRII male mice were treated with either galunisertib and enzalutamide, in combination or as single agents in three "mini"-trials and the effects on tumor growth, phenotypic EMT, and actin cytoskeleton were evaluated. RESULTS: Galunisertib in combination with enzalutamide significantly suppressed prostate tumor growth, by increasing apoptosis and decreasing cell proliferation of tumor cell populations compared to the inhibitor as a monotherapy (P < 0.05). The combination treatment dramatically reduced cofilin levels, actin cytoskeleton regulator, compared to single agents. Treatment with galunisertib targeted nuclear Smad4 protein (intracellular TGF-β effector), but had no effect on nuclear AR. Consequential to TGF-β inhibition there was an EMT reversion to mesenchymal-epithelial transition (MET) and re-differentiation of prostate tumors. Elevated intratumoral TGF-β1 ligand, in response to galunisertib, was blocked by enzalutamide. CONCLUSION: Our results provide novel insights into the therapeutic value of targeting TGF-β signaling to overcome resistance to enzalutamide in prostate cancer by phenotypic reprogramming of EMT towards tumor re-differentiation and cytoskeleton remodeling. This translational work is significant in sequencing TGF-β blockade and antiandrogens to optimize therapeutic response in CRPC.
BACKGROUND:Prostate cancer progression is navigated by the androgen receptor (AR) and transforming-growth factor-β (TGF-β) signaling. We previously demonstrated that aberrant TGF-β signaling accelerates prostate tumor progression in a transgenic mouse model of prostate cancer via effects on epithelial-mesenchymal transition (EMT), driving castration-resistant prostate cancer (CRPC). METHODS: This study examined the antitumor effect of the combination of TGF-β receptor I (TβRI) inhibitor, galunisertib, and FDA-approved antiandrogen enzalutamide, in our pre-clinical model. Age-matched genotypically characterized DNTGFβRII male mice were treated with either galunisertib and enzalutamide, in combination or as single agents in three "mini"-trials and the effects on tumor growth, phenotypic EMT, and actin cytoskeleton were evaluated. RESULTS:Galunisertib in combination with enzalutamide significantly suppressed prostate tumor growth, by increasing apoptosis and decreasing cell proliferation of tumor cell populations compared to the inhibitor as a monotherapy (P < 0.05). The combination treatment dramatically reduced cofilin levels, actin cytoskeleton regulator, compared to single agents. Treatment with galunisertib targeted nuclear Smad4 protein (intracellular TGF-β effector), but had no effect on nuclear AR. Consequential to TGF-β inhibition there was an EMT reversion to mesenchymal-epithelial transition (MET) and re-differentiation of prostate tumors. Elevated intratumoral TGF-β1 ligand, in response to galunisertib, was blocked by enzalutamide. CONCLUSION: Our results provide novel insights into the therapeutic value of targeting TGF-β signaling to overcome resistance to enzalutamide in prostate cancer by phenotypic reprogramming of EMT towards tumor re-differentiation and cytoskeleton remodeling. This translational work is significant in sequencing TGF-β blockade and antiandrogens to optimize therapeutic response in CRPC.
Authors: Yara Rodríguez; Kenji Unno; Mihai I Truica; Zachary R Chalmers; Young A Yoo; Rajita Vatapalli; Vinay Sagar; Jindan Yu; Barbara Lysy; Maha Hussain; Huiying Han; Sarki A Abdulkadir Journal: Cancer Res Date: 2022-06-06 Impact factor: 13.312
Authors: Gaelle Fiard; Vasilis Stavrinides; Emma S Chambers; Susan Heavey; Alex Freeman; Rhys Ball; Arne N Akbar; Mark Emberton Journal: Nat Rev Urol Date: 2021-07-22 Impact factor: 14.432
Authors: Patrick J Hensley; Natasha Kyprianou; Matthew S Purdom; Daheng He; Vincent DiCarlo; Chi Wang; Andrew C James Journal: Urol Oncol Date: 2019-07-17 Impact factor: 2.954
Authors: Joshi J Alumkal; Duanchen Sun; Eric Lu; Tomasz M Beer; George V Thomas; Emile Latour; Rahul Aggarwal; Jeremy Cetnar; Charles J Ryan; Shaadi Tabatabaei; Shawna Bailey; Claire B Turina; David A Quigley; Xiangnan Guan; Adam Foye; Jack F Youngren; Joshua Urrutia; Jiaoti Huang; Alana S Weinstein; Verena Friedl; Matthew Rettig; Robert E Reiter; Daniel E Spratt; Martin Gleave; Christopher P Evans; Joshua M Stuart; Yiyi Chen; Felix Y Feng; Eric J Small; Owen N Witte; Zheng Xia Journal: Proc Natl Acad Sci U S A Date: 2020-05-18 Impact factor: 11.205