Targeting Bromodomain and Extra-Terminal (BET) Family Proteins in Castration-Resistant Prostate Cancer (CRPC)

Welti, Jonathan; Sharp, Adam; Yuan, Wei; Dolling, David; Rodrigues, Daniel Nava; Figueiredo, Ines; Gil, Veronica; Neeb, Antje; Clarke, Matthew; Seed, George; Crespo, Mateus; Sumanasuriya, Semini; Ning, Jian; Knight, Eleanor; Francis, Jeffrey C.; Hughes, Ashley M.; Halsey, Wendy S.; Paschalis, Alec; Mani, Ram S.; Raj, Ganesh V.; Plymate, Stephen R.; Carreira, Suzanne; Boysen, Gunther; Chinnaiyan, Arul M.; Swain, Amanda; Bono, Johann S. de

doi:10.1158/1078-0432.ccr-17-3571

Cited by 118 publications

(106 citation statements)

References 50 publications

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“…Moreover, high BRD2 expression in primary tumors was associated with shorter PC-specific survival . More recently, the nuclear BRD4 protein level was confirmed to increase following castration resistance in longitudinally matched tumor samples collected pre and post treatment (Welti et al 2018). We also found that high expression of ATAD2 was positively associated with biochemical recurrence on a cohort of 10,000 patients .…”

Section: Bromodomain-containing Proteins and Chromatin Reprogramming supporting

confidence: 63%

Chromatin reprogramming as an adaptation mechanism in advanced prostate cancer

Braadland

Urbanucci

2019

Endocrine-Related Cancer

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Tumor evolution is based on the ability to constantly mutate and activate different pathways under the selective pressure of targeted therapies. Epigenetic alterations including those of the chromatin structure are associated with tumor initiation, progression and drug resistance. Many cancers, including prostate cancer, present enlarged nuclei, and chromatin appears altered and irregular. These phenotypic changes are likely to result from epigenetic dysregulation. High-throughput sequencing applied to bulk samples and now to single cells has made it possible to study these processes in unprecedented detail. It is therefore timely to review the impact of chromatin relaxation and increased DNA accessibility on prostate cancer growth and drug resistance, and their effects on gene expression. In particular, we focus on the contribution of chromatinassociated proteins such as the bromodomain-containing proteins to chromatin relaxation. We discuss the consequence of this for androgen receptor transcriptional activity and briefly summarize wider gain-of-function effects on other oncogenic transcription factors and implications for more effective prostate cancer treatment.

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Section: Bromodomain-containing Proteins and Chromatin Reprogramming supporting

confidence: 63%

Chromatin reprogramming as an adaptation mechanism in advanced prostate cancer

Braadland

Urbanucci

2019

Endocrine-Related Cancer

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“…Transcriptional signatures from intermediate adenocarcinoma patients overlapped with datasets from neuroendocrine prostate cancer patients, suggesting that in the context of retained AR function, tumors can also activate lineage plasticity networks to evade ADT without shutting down AR expression. Evidence of this exists where enzalutamideresistant preclinical models with AR expression have shown benefit from disruption of bromo-and extraterminal domain (BET) bromodomain proteins by BET inhibitors (14,15). Overall, BET inhibitors enhanced efficacy and reversed resistance to AR antagonists.…”

mentioning

confidence: 99%

LSD1: A single target to combat lineage plasticity in lethal prostate cancer

Ellis

Loda

2018

Proc. Natl. Acad. Sci. U.S.A.

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“…Epigenetic drugs targeting the BET family of chromatin readers and transcriptional regulators, such as BRD4, are also in clinical development. Pre-clinical studies have shown that drugs targeting BRD4 disrupt its recruitment to chromatin sites bound by AR, suppress signaling, and, alone or in combination with ARPIs, demonstrate anti-tumour activity (Asangani et al 2014, Welti et al 2018. This is due, in part,to the requirement of BRD4 activity to mediate chromatin accessibility and AR transcriptional reprogramming during prostate cancer progression (Urbanucci et al 2017).…”

Section: Targeting Epigenetic and Transcriptional Regulators In Nepcmentioning

confidence: 99%

The epigenetic and transcriptional landscape of neuroendocrine prostate cancer

Davies

Zoubeidi

Selth

2020

Endocrine-Related Cancer

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Tumours adapt to increasingly potent targeted therapies by transitioning to alternative lineage states. In prostate cancer, the widespread clinical application of androgen receptor (AR) pathway inhibitors has led to the insurgence of tumours relapsing with a neuroendocrine phenotype, termed neuroendocrine prostate cancer (NEPC). Recent evidence suggests that this lineage reprogramming is driven largely by dysregulation of the epigenome and transcriptional networks. Indeed, aberrant DNA methylation patterning and altered expression of epigenetic modifiers, such as EZH2, transcription factors, and RNA-modifying factors, are hallmarks of NEPC tumours. In this review, we explore the nature of the epigenetic and transcriptional landscape as prostate cancer cells lose their AR-imposed identity and transition to the neuroendocrine lineage. Beyond addressing the mechanisms underlying epithelial-to-neuroendocrine lineage reprogramming, we discuss how oncogenic signaling and metabolic shifts fuel epigenetic/transcriptional changes as well as the current state of epigenetic therapies for NEPC.

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Targeting Bromodomain and Extra-Terminal (BET) Family Proteins in Castration-Resistant Prostate Cancer (CRPC)

Cited by 118 publications

References 50 publications

Chromatin reprogramming as an adaptation mechanism in advanced prostate cancer

Chromatin reprogramming as an adaptation mechanism in advanced prostate cancer

LSD1: A single target to combat lineage plasticity in lethal prostate cancer

The epigenetic and transcriptional landscape of neuroendocrine prostate cancer

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