Targeted inhibition of ERα signaling and PIP5K1α/Akt pathways in castration‐resistant prostate cancer

Julius Semenas; Tianyan Wang; Azharuddin Sajid Syed Khaja; AKM Firoj Mahmud; Athanasios Simoulis; Thomas Grundström; Maria Fällman; Jenny L. Persson

doi:10.1002/1878-0261.12873

Molecular Oncology (Apr 2021)

Targeted inhibition of ERα signaling and PIP5K1α/Akt pathways in castration‐resistant prostate cancer

Julius Semenas,
Tianyan Wang,
Azharuddin Sajid Syed Khaja,
AKM Firoj Mahmud,
Athanasios Simoulis,
Thomas Grundström,
Maria Fällman,
Jenny L. Persson

Affiliations

Julius Semenas: Department of Molecular Biology Umeå University Sweden
Tianyan Wang: Department of Molecular Biology Umeå University Sweden
Azharuddin Sajid Syed Khaja: Department of Molecular Biology Umeå University Sweden
AKM Firoj Mahmud: Department of Molecular Biology Umeå University Sweden
Athanasios Simoulis: Department of Clinical Pathology and Cytology Skåne University Hospital Malmö Sweden
Thomas Grundström: Department of Molecular Biology Umeå University Sweden
Maria Fällman: Department of Molecular Biology Umeå University Sweden
Jenny L. Persson: Department of Molecular Biology Umeå University Sweden

DOI: https://doi.org/10.1002/1878-0261.12873
Journal volume & issue: Vol. 15, no. 4
pp. 968 – 986

Abstract

Read online

Selective ERα modulator, tamoxifen, is well tolerated in a heavily pretreated castration‐resistant prostate cancer (PCa) patient cohort. However, its targeted gene network and whether expression of intratumor ERα due to androgen deprivation therapy (ADT) may play a role in PCa progression is unknown. In this study, we examined the inhibitory effect of tamoxifen on castration‐resistant PCa in vitro and in vivo. We found that tamoxifen is a potent compound that induced a high degree of apoptosis and significantly suppressed growth of xenograft tumors in mice, at a degree comparable to ISA‐2011B, an inhibitor of PIP5K1α that acts upstream of PI3K/AKT survival signaling pathway. Moreover, depletion of tumor‐associated macrophages using clodronate in combination with tamoxifen increased inhibitory effect of tamoxifen on aggressive prostate tumors. We showed that both tamoxifen and ISA‐2011B exert their on‐target effects on prostate cancer cells by targeting cyclin D1 and PIP5K1α/AKT network and the interlinked estrogen signaling. Combination treatment using tamoxifen together with ISA‐2011B resulted in tumor regression and had superior inhibitory effect compared with that of tamoxifen or ISA‐2011B alone. We have identified sets of genes that are specifically targeted by tamoxifen, ISA‐2011B or combination of both agents by RNA‐seq. We discovered that alterations in unique gene signatures, in particular estrogen‐related marker genes are associated with poor patient disease‐free survival. We further showed that ERα interacted with PIP5K1α through formation of protein complexes in the nucleus, suggesting a functional link. Our finding is the first to suggest a new therapeutic potential to inhibit or utilize the mechanisms related to ERα, PIP5K1α/AKT network, and MMP9/VEGF signaling axis, providing a strategy to treat castration‐resistant ER‐positive subtype of prostate cancer tumors with metastatic potential.

Published in Molecular Oncology

ISSN: 1574-7891 (Print); 1878-0261 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://febs.onlinelibrary.wiley.com/journal/18780261

About the journal

Abstract

Keywords