Knocking down AR promotes osteoblasts to recruit prostate cancer cells by altering exosomal circ-DHPS/miR-214-3p/CCL5 pathway

Zhao Yang; Jia-Qi Chen; Tian-Jie Liu; Yu-Le Chen; Zhen-Kun Ma; Yi-Zeng Fan; Zi-Xi Wang; Shan Xu; Ke Wang; Xin-Yang Wang; Lei Li; Hong-Jun Xie

doi:10.4103/aja202351

Knocking down AR promotes osteoblasts to recruit prostate cancer cells by altering exosomal circ-DHPS/miR-214-3p/CCL5 pathway

Asian J Androl. 2023 Nov 14;26(2):195-204. doi: 10.4103/aja202351. Online ahead of print.

Authors

Zhao Yang¹, Jia-Qi Chen, Tian-Jie Liu, Yu-Le Chen, Zhen-Kun Ma, Yi-Zeng Fan, Zi-Xi Wang, Shan Xu, Ke Wang, Xin-Yang Wang, Lei Li, Hong-Jun Xie

Affiliation

¹ Department of Urology, The First Affiliated Hospital of Xi'an Jiaotong University, Xi'an 710061, China.

Abstract

Tumor-derived exosomes have been shown to play a key role in organ-specific metastasis, and the androgen receptor regulates prostate cancer (PCa) progression. It is unclear whether the androgen receptor regulates the recruitment of prostate cancer cells to the bone microenvironment, even bone metastases, through exosomes. Here, we found that exosomes isolated from PCa cells after knocking down androgen receptor (AR) or enzalutamide treatment can facilitate the migration of prostate cancer cells to osteoblasts. In addition, AR silencing or treatment with the AR antagonist enzalutamide may increase the expression of circular RNA-deoxyhypusine synthase (circ-DHPS) in PCa cells, which can be transported to osteoblasts by exosomes. Circ-DHPS acts as a competitive endogenous RNA (ceRNA) against endogenous miR-214-3p to promote C-C chemokine ligand 5 (CCL5) levels in osteoblasts. Increasing the level of CCL5 in osteoblasts could recruit more PCa cells into the bone microenvironment. Thus, blocking the circ-DHPS/miR-214-3p/CCL5 signal may decrease exosome-mediated migration of prostate cancer cells to osteoblasts.