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

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

Mol Oncol. 2021 Apr;15(4):968-986. doi: 10.1002/1878-0261.12873. Epub 2020 Dec 16.

Authors

Julius Semenas¹, Tianyan Wang¹, Azharuddin Sajid Syed Khaja¹, Akm Firoj Mahmud¹, Athanasios Simoulis², Thomas Grundström¹, Maria Fällman¹, Jenny L Persson^{1

3

4}

Affiliations

¹ Department of Molecular Biology, Umeå University, Sweden.
² Department of Clinical Pathology and Cytology, Skåne University Hospital, Malmö, Sweden.
³ Division of Experimental Cancer Research, Department of Translational Medicine, Lund University, Clinical Research Centre in Malmö, Sweden.
⁴ Department of Biomedical Science, Malmö University, Sweden.

Abstract

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.

Keywords: PI3K/AKT pathway and tamoxifen; PIP5K1α; castration-resistant prostate cancer; estrogen receptor; targeted therapy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Apoptosis
Diketopiperazines / therapeutic use*
Estrogen Receptor alpha / antagonists & inhibitors*
Humans
Indoles / therapeutic use*
Isoquinolines / therapeutic use*
Male
Mice
Mice, Nude
PC-3 Cells
Phosphotransferases (Alcohol Group Acceptor) / antagonists & inhibitors
Prostatic Neoplasms, Castration-Resistant / drug therapy*
Proto-Oncogene Proteins c-akt
RNA-Seq
Signal Transduction / drug effects*
Tamoxifen / therapeutic use*
Xenograft Model Antitumor Assays

Substances

Diketopiperazines
ESR1 protein, human
Estrogen Receptor alpha
ISA-2011B
Indoles
Isoquinolines
Tamoxifen
Phosphotransferases (Alcohol Group Acceptor)
1-phosphatidylinositol-4-phosphate 5-kinase
Proto-Oncogene Proteins c-akt