Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation

Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation

Prostate cancer (PCa) is one of the most frequent tumor types in the male Western population. Early‐stage PCa and late‐stage PCa are dependent on androgen signaling, and inhibitors of the androgen receptor (AR) axis represent the standard therapy. Here, we studied in detail the global impact of daro...

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Main Authors: Simon J. Baumgart, Ekaterina Nevedomskaya, Ralf Lesche, Richard Newman, Dominik Mumberg, Bernard Haendler
Format: Article
Language:English
Published: Wiley 2020-09-01
Series:Molecular Oncology
Subjects:
androgen receptor
cistrome
FOXA1
histone acetylation
prostate cancer
super‐enhancer
Online Access:https://doi.org/10.1002/1878-0261.12693
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spelling doaj-86eb25843f434d4ba5497af7a5b7dd5f2020-11-25T03:17:08ZengWileyMolecular Oncology1574-78911878-02612020-09-011492022203910.1002/1878-0261.12693Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activationSimon J. Baumgart0Ekaterina Nevedomskaya1Ralf Lesche2Richard Newman3Dominik Mumberg4Bernard Haendler5Research and Development, Pharmaceuticals Bayer AG Berlin GermanyResearch and Development, Pharmaceuticals Bayer AG Berlin GermanyResearch and Development, Pharmaceuticals Bayer AG Berlin GermanyResearch and Development, Pharmaceuticals Bayer AG Berlin GermanyResearch and Development, Pharmaceuticals Bayer AG Berlin GermanyResearch and Development, Pharmaceuticals Bayer AG Berlin GermanyProstate cancer (PCa) is one of the most frequent tumor types in the male Western population. Early‐stage PCa and late‐stage PCa are dependent on androgen signaling, and inhibitors of the androgen receptor (AR) axis represent the standard therapy. Here, we studied in detail the global impact of darolutamide, a newly approved AR antagonist, on the transcriptome and AR‐bound cistrome in two PCa cell models. Darolutamide strongly depleted the AR from gene regulatory regions and abolished AR‐driven transcriptional signaling. Enhancer activation was blocked at the chromatin level as evaluated by H3K27 acetylation (H3K27ac), H3K4 monomethylation (H3K4me1), and FOXA1, MED1, and BRD4 binding. We identified genomic regions with high affinities for the AR in androgen‐stimulated, but also in androgen‐depleted conditions. A similar AR affinity pattern was observed in healthy and PCa tissue samples. High FOXA1, BRD4, H3K27ac, and H3K4me1 levels were found to mark regions showing AR binding in the hormone‐depleted setting. Conversely, low FOXA1, BRD4, and H3K27ac levels were observed at regulatory sites that responded strongly to androgen stimulation, and AR interactions at these sites were blocked by darolutamide. Beside marked loss of AR occupancy, FOXA1 recruitment to chromatin was also clearly reduced after darolutamide treatment. We furthermore identified numerous androgen‐regulated super‐enhancers (SEs) that were associated with hallmark androgen and cell proliferation‐associated gene sets. Importantly, these SEs are also active in PCa tissues and sensitive to darolutamide treatment in our models. Our findings demonstrate that darolutamide is a potent AR antagonist blocking genome‐wide AR enhancer and SE activation, and downstream transcription. We also show the existence of a dynamic AR cistrome that depends on the androgen levels and on high AR affinity regions present in PCa cell lines and also in tissue samples.https://doi.org/10.1002/1878-0261.12693androgen receptorcistromeFOXA1histone acetylationprostate cancersuper‐enhancer
collection DOAJ
language English
format Article
sources DOAJ
author Simon J. Baumgart
Ekaterina Nevedomskaya
Ralf Lesche
Richard Newman
Dominik Mumberg
Bernard Haendler
spellingShingle Simon J. Baumgart
Ekaterina Nevedomskaya
Ralf Lesche
Richard Newman
Dominik Mumberg
Bernard Haendler
Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation
Molecular Oncology
androgen receptor
cistrome
FOXA1
histone acetylation
prostate cancer
super‐enhancer
author_facet Simon J. Baumgart
Ekaterina Nevedomskaya
Ralf Lesche
Richard Newman
Dominik Mumberg
Bernard Haendler
author_sort Simon J. Baumgart
title Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation
title_short Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation
title_full Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation
title_fullStr Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation
title_full_unstemmed Darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation
title_sort darolutamide antagonizes androgen signaling by blocking enhancer and super‐enhancer activation
publisher Wiley
series Molecular Oncology
issn 1574-7891
1878-0261
publishDate 2020-09-01
description Prostate cancer (PCa) is one of the most frequent tumor types in the male Western population. Early‐stage PCa and late‐stage PCa are dependent on androgen signaling, and inhibitors of the androgen receptor (AR) axis represent the standard therapy. Here, we studied in detail the global impact of darolutamide, a newly approved AR antagonist, on the transcriptome and AR‐bound cistrome in two PCa cell models. Darolutamide strongly depleted the AR from gene regulatory regions and abolished AR‐driven transcriptional signaling. Enhancer activation was blocked at the chromatin level as evaluated by H3K27 acetylation (H3K27ac), H3K4 monomethylation (H3K4me1), and FOXA1, MED1, and BRD4 binding. We identified genomic regions with high affinities for the AR in androgen‐stimulated, but also in androgen‐depleted conditions. A similar AR affinity pattern was observed in healthy and PCa tissue samples. High FOXA1, BRD4, H3K27ac, and H3K4me1 levels were found to mark regions showing AR binding in the hormone‐depleted setting. Conversely, low FOXA1, BRD4, and H3K27ac levels were observed at regulatory sites that responded strongly to androgen stimulation, and AR interactions at these sites were blocked by darolutamide. Beside marked loss of AR occupancy, FOXA1 recruitment to chromatin was also clearly reduced after darolutamide treatment. We furthermore identified numerous androgen‐regulated super‐enhancers (SEs) that were associated with hallmark androgen and cell proliferation‐associated gene sets. Importantly, these SEs are also active in PCa tissues and sensitive to darolutamide treatment in our models. Our findings demonstrate that darolutamide is a potent AR antagonist blocking genome‐wide AR enhancer and SE activation, and downstream transcription. We also show the existence of a dynamic AR cistrome that depends on the androgen levels and on high AR affinity regions present in PCa cell lines and also in tissue samples.
topic androgen receptor
cistrome
FOXA1
histone acetylation
prostate cancer
super‐enhancer
url https://doi.org/10.1002/1878-0261.12693
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