Retinoic Acid Receptor Activation Reduces Metastatic Prostate Cancer Bone Lesions by Blocking the Endothelial-to-Osteoblast Transition

Guoyu Yu; Paul G Corn; Pengfei Shen; Jian H Song; Yu-Chen Lee; Song-Chang Lin; Jing Pan; Sandeep K Agarwal; Theocharis Panaretakis; Maurizio Pacifici; Christopher J Logothetis; Li-Yuan Yu-Lee; Sue-Hwa Lin

doi:10.1158/0008-5472.CAN-22-0170

Retinoic Acid Receptor Activation Reduces Metastatic Prostate Cancer Bone Lesions by Blocking the Endothelial-to-Osteoblast Transition

Cancer Res. 2022 Sep 2;82(17):3158-3171. doi: 10.1158/0008-5472.CAN-22-0170.

Authors

Affiliations

¹ Department of Translational Molecular Pathology, The University of Texas M. D. Anderson Cancer Center; Houston, Texas.
² Department of Genitourinary Medical Oncology, The University of Texas M. D. Anderson Cancer Center, Houston, Texas.
³ Department of Medicine, Section of Immunology Allergy & Rheumatology, Baylor College of Medicine, Houston, Texas.
⁴ Translational Research Program in Pediatric Orthopaedics, The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania.
⁵ The University of Texas Graduate School of Biomedical Sciences at Houston, Houston, Texas.

^# Contributed equally.

Abstract

Metastatic prostate cancer in the bone induces bone-forming lesions that contribute to progression and therapy resistance. Prostate cancer-induced bone formation originates from endothelial cells (EC) that have undergone endothelial-to-osteoblast (EC-to-OSB) transition in response to tumor-secreted BMP4. Current strategies targeting prostate cancer-induced bone formation are lacking. Here, we show that activation of retinoic acid receptor (RAR) inhibits EC-to-OSB transition and reduces prostate cancer-induced bone formation. Treatment with palovarotene, an RARγ agonist being tested for heterotopic ossification in fibrodysplasia ossificans progressiva, inhibited EC-to-OSB transition and osteoblast mineralization in vitro and decreased tumor-induced bone formation and tumor growth in several osteogenic prostate cancer models, and similar effects were observed with the pan-RAR agonist all-trans-retinoic acid (ATRA). Knockdown of RARα, β, or γ isoforms in ECs blocked BMP4-induced EC-to-OSB transition and osteoblast mineralization, indicating a role for all three isoforms in prostate cancer-induced bone formation. Furthermore, treatment with palovarotene or ATRA reduced plasma Tenascin C, a factor secreted from EC-OSB cells, which may be used to monitor treatment response. Mechanistically, BMP4-activated pSmad1 formed a complex with RAR in the nucleus of ECs to activate EC-to-OSB transition. RAR activation by palovarotene or ATRA caused pSmad1 degradation by recruiting the E3-ubiquitin ligase Smad ubiquitination regulatory factor1 (Smurf1) to the nuclear pSmad1/RARγ complex, thus blocking EC-to-OSB transition. Collectively, these findings suggest that palovarotene can be repurposed to target prostate cancer-induced bone formation to improve clinical outcomes for patients with bone metastasis.

Significance: This study provides mechanistic insights into how RAR agonists suppress prostate cancer-induced bone formation and offers a rationale for developing RAR agonists for prostate cancer bone metastasis therapy. See related commentary by Bhowmick and Bhowmick, p. 2975.

Publication types

Research Support, Non-U.S. Gov't
Research Support, N.I.H., Extramural

MeSH terms

Bone Neoplasms* / metabolism
Endothelial Cells / pathology
Humans
Male
Osteoblasts / metabolism
Prostatic Neoplasms* / pathology
Receptors, Retinoic Acid / metabolism
Tretinoin / metabolism
Tretinoin / pharmacology
Ubiquitin-Protein Ligases / metabolism

Substances

Receptors, Retinoic Acid
Tretinoin
SMURF1 protein, human
Ubiquitin-Protein Ligases

Abstract

Publication types

MeSH terms

Substances

Grants and funding