Wntless promotes cellular viability and resistance to enzalutamide in castration-resistant prostate cancer cells

Alan P Lombard; Chengfei Liu; Cameron M Armstrong; Leandro S D'Abronzo; Wei Lou; Christopher P Evans; Allen C Gao

Wntless promotes cellular viability and resistance to enzalutamide in castration-resistant prostate cancer cells

Am J Clin Exp Urol. 2019 Aug 15;7(4):203-214. eCollection 2019.

Authors

Alan P Lombard¹, Chengfei Liu¹, Cameron M Armstrong¹, Leandro S D'Abronzo¹, Wei Lou¹, Christopher P Evans^{1

2}, Allen C Gao^{1

2

3}

Affiliations

¹ Department of Urologic Surgery, University of California Davis CA, USA.
² UC Davis Comprehensive Cancer Center, University of California Davis CA, USA.
³ VA Northern California Health Care System Sacramento, CA, USA.

PMID: 31511827
PMCID: PMC6734040

Abstract

Background: De-regulation of Wnt signaling pathways has been shown to be associated with progression of castration-resistant prostate cancer and more recently, studies indicate that both canonical and non-canonical Wnt pathways may mediate resistance to anti-androgen therapies such as enzalutamide. However, the mechanisms by which Wnt signaling is altered in prostate cancer remain poorly understood. Wnt pathway function begins with Wnt biogenesis and secretion from Wnt signal sending cells. While previous studies have investigated downstream mechanisms of Wnt pathway alterations in prostate cancer, little is known on the role of Wnt secretion mediating proteins. Wntless (WLS) is thought to be essential for the secretion of all Wnts. In this study, we sought to understand the role of WLS in prostate cancer.

Methods: RNA-seq and gene set enrichment analysis were used to understand expression profile changes in enzalutamide-resistant C4-2B-MDVR (MDVR) cells versus parental C4-2B cells. Quantitative-PCR and western blot were used to confirm RNA-seq data and to assess expression changes of gene targets of interest. Rv1 cells were used as a separate model of enzalutamide-resistant prostate cancer. RNAi was used to inhibit WLS expression. Cell viability, colony formation, and PSA ELISA assays were used to assess cell growth and survival.

Results: Transcriptomic profiling revealed enriched Wnt pathway signatures in MDVR versus parental C4-2B cells. We further show that MDVR cells upregulate Wnt signaling and overexpress WLS. Inhibition of WLS decreases Wnt signaling, markedly attenuates prostate cancer cell viability, induces apoptosis, and re-sensitizes enzalutamide-resistant cells to enzalutamide treatment. Lastly, we show that inhibition of WLS reduces AR and AR-variants expression and downstream signaling.

Conclusions: Our findings support a role for WLS in the progression of prostate cancer to a treatment-resistant state. Further efforts to understand Wnt signaling pathway alterations in this disease may lead to the development of novel treatments.

Keywords: Wnt signaling; castration-resistant prostate cancer; enzalutamide resistance; porcn; porcupine; wls; wntless.