NR5A2/HSD3B1 pathway promotes cellular resistance to second-generation antiandrogen darolutamide

NR5A2/HSD3B1 pathway promotes cellular resistance to second-generation antiandrogen darolutamide

This study investigated cellular mechanisms in steroidogenesis responsible for treatment resistance to the novel antiandrogen agent darolutamide in prostate cancer. HSD3B1 was overexpressed in darolutamide-resistant cells and induced by darolutamide treatment and AR knockdown. Inversely, HSD3B1 knoc...

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Veröffentlicht in:Drug resistance updates 2023-09, Vol.70, p.100990-100990, Article 100990
Hauptverfasser: Shiota, Masaki, Ushijima, Miho, Tsukahara, Shigehiro, Nagakawa, Shohei, Blas, Leandro, Takamatsu, Dai, Kobayashi, Satoshi, Matsumoto, Takashi, Inokuchi, Junichi, Eto, Masatoshi
Format: Artikel
Sprache:eng
Schlagworte:
Androgen-deprivation therapy
Darolutamide
HSD3B1
NR5A2
Prostate cancer
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Zusammenfassung:This study investigated cellular mechanisms in steroidogenesis responsible for treatment resistance to the novel antiandrogen agent darolutamide in prostate cancer. HSD3B1 was overexpressed in darolutamide-resistant cells and induced by darolutamide treatment and AR knockdown. Inversely, HSD3B1 knockdown increased cellular sensitivity to darolutamide. Similarly, its upstream regulator NR5A2 was up-regulated in darolutamide-resistant cells and induced by darolutamide treatment and AR knockdown. Inversely, NR5A2 knockdown and NR5A2 inhibitor ML180 decreased expression of various steroidogenic enzymes including HSD3B1, leading to increased cellular sensitivity to darolutamide. The NR5A2/HSD3B1 pathway promoted cellular resistance to darolutamide and targeting NR5A2/HSD3B1 pathway is a promising therapeutic strategy to overcome darolutamide resistance.
ISSN:1368-7646
1532-2084
DOI:10.1016/j.drup.2023.100990