Retinoic Acid Receptor Activation Reduces Metastatic Prostate Cancer Bone Lesions by Blocking the Endothelial-to-Osteoblast Transition-Reference-Cited by-同舟云学术

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

Published:2022-07-08 Issue:17 Volume:82 Page:3158-3171
ISSN:0008-5472
Container-title:Cancer Research
language:en
Short-container-title:

Author:

Yu Guoyu¹,Corn Paul G.²,Shen Pengfei¹^ORCID,Song Jian H.²,Lee Yu-Chen¹,Lin Song-Chang¹,Pan Jing²,Agarwal Sandeep K.³^ORCID,Panaretakis Theocharis²^ORCID,Pacifici Maurizio⁴,Logothetis Christopher J.²^ORCID,Yu-Lee Li-Yuan³^ORCID,Lin Sue-Hwa¹²⁵^ORCID

Affiliation:

1. 1Department of Translational Molecular Pathology, The University of Texas M. D. Anderson Cancer Center; Houston, Texas.

2. 2Department of Genitourinary Medical Oncology, The University of Texas M. D. Anderson Cancer Center, Houston, Texas.

3. 3Department of Medicine, Section of Immunology Allergy & Rheumatology, Baylor College of Medicine, Houston, Texas.

4. 4Translational Research Program in Pediatric Orthopaedics, The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania.

5. 5The University of Texas Graduate School of Biomedical Sciences at Houston, Houston, Texas.

Abstract

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

Funder

NIH

Cancer Prevention and Research Institute of Texas

CPRIT

Biology of Inflammation Center Arthritis Research Endowment

Publisher

American Association for Cancer Research (AACR)

Subject

Cancer Research,Oncology

Link

https://aacrjournals.org/cancerres/article-pdf/doi/10.1158/0008-5472.CAN-22-0170/3179462/can-22-0170.pdf

Reference61 articles.