Reversible epigenetic alterations mediate PSMA expression heterogeneity in advanced metastatic prostate cancer
Erolcan Sayar, Radhika A. Patel, Ilsa M. Coleman, Martine P. Roudier, Ailin Zhang, Pallabi Mustafi, Jin-Yih Low, Brian Hanratty, Lisa S. Ang, Vipul Bhatia, Mohamed Adil, Hasim Bakbak, David A. Quigley, Michael T. Schweizer, Jessica E. Hawley, Lori Kollath, Lawrence D. True, Felix Y. Feng, Neil H. Bander, Eva Corey, John K. Lee, Colm Morrissey, Roman Gulati, Peter S. Nelson, Michael C. Haffner
Erolcan Sayar, Radhika A. Patel, Ilsa M. Coleman, Martine P. Roudier, Ailin Zhang, Pallabi Mustafi, Jin-Yih Low, Brian Hanratty, Lisa S. Ang, Vipul Bhatia, Mohamed Adil, Hasim Bakbak, David A. Quigley, Michael T. Schweizer, Jessica E. Hawley, Lori Kollath, Lawrence D. True, Felix Y. Feng, Neil H. Bander, Eva Corey, John K. Lee, Colm Morrissey, Roman Gulati, Peter S. Nelson, Michael C. Haffner
View: Text | PDF
Research Article Oncology

Reversible epigenetic alterations mediate PSMA expression heterogeneity in advanced metastatic prostate cancer

Abstract

Prostate-specific membrane antigen (PSMA) is an important cell surface target in prostate cancer. There are limited data on the heterogeneity of PSMA tissue expression in metastatic castration-resistant prostate cancer (mCRPC). Furthermore, the mechanisms regulating PSMA expression (encoded by the FOLH1 gene) are not well understood. Here, we demonstrate that PSMA expression is heterogeneous across different metastatic sites and molecular subtypes of mCRPC. In a rapid autopsy cohort in which multiple metastatic sites per patient were sampled, we found that 13 of 52 (25%) cases had no detectable PSMA and 23 of 52 (44%) cases showed heterogeneous PSMA expression across individual metastases, with 33 (63%) cases harboring at least 1 PSMA-negative site. PSMA-negative tumors displayed distinct transcriptional profiles with expression of druggable targets such as MUC1. Loss of PSMA was associated with epigenetic changes of the FOLH1 locus, including gain of CpG methylation and loss of histone 3 lysine 27 (H3K27) acetylation. Treatment with histone deacetylase (HDAC) inhibitors reversed this epigenetic repression and restored PSMA expression in vitro and in vivo. Collectively, these data provide insights into the expression patterns and regulation of PSMA in mCRPC and suggest that epigenetic therapies — in particular, HDAC inhibitors — can be used to augment PSMA levels.

Authors

Erolcan Sayar, Radhika A. Patel, Ilsa M. Coleman, Martine P. Roudier, Ailin Zhang, Pallabi Mustafi, Jin-Yih Low, Brian Hanratty, Lisa S. Ang, Vipul Bhatia, Mohamed Adil, Hasim Bakbak, David A. Quigley, Michael T. Schweizer, Jessica E. Hawley, Lori Kollath, Lawrence D. True, Felix Y. Feng, Neil H. Bander, Eva Corey, John K. Lee, Colm Morrissey, Roman Gulati, Peter S. Nelson, Michael C. Haffner

×

Figure 3

Tumors with low/negative PSMA expression show distinct expression changes.

Options: View larger image (or click on image) Download as PowerPoint
Tumors with low/negative PSMA expression show distinct expression change...
(A and B) Heatmap showing the top 50 genes upregulated in AR+/NE tumors from the LuCaP PDX (n = 82), UW-TAN (n = 109), and SU2C (n = 182) cohorts with low/negative PSMA expression (A) and high PSMA expression (B). (C and D) Gene set enrichment analyses using Hallmark Pathways (C) and KEGG Pathways (D) show gene sets enriched in PSMA high (red) and PSMA-low/negative (blue) tumors. NES denotes normalized enrichment score. (E and F) Comparisons of AR signaling activity (AR-score) and cell proliferation (CCP-score) using gene set variation analyses (Supplemental Figures 12 and 13) between PSMA-low/negative and PSMA-high AR+/NE tumors in the UW-TAN (E) and SU2C (F) cohorts. (G and H) CIBERSORTx analyses demonstrate differences in macrophage infiltration between PSMA high and PSMA low/negative tumors in UW-TAN (G) and SU2C (H) cohorts. (I and J) Differences in PSMA expression based on luminal A, luminal B, and basal PAM-50 status in UW-TAN (I) and SU2C (J) cohorts. P values are based Wilcoxon rank tests.