PROTAC-induced BET protein degradation as a therapy for castration-resistant prostate cancer

Raina, Kanak; Lü, Jing; Qian, Yimin; Altieri, Martha; Gordon, Deborah; Rossi, Ann Marie; Wang, Jing; Chen, Xin; Dong, Hanqing; Siu, Kam; Winkler, James D.; Crew, Andrew P.; Crews, Craig M.; Coleman, Kevin

doi:10.1073/pnas.1521738113

Cited by 686 publications

(698 citation statements)

References 45 publications

(65 reference statements)

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“…One promising strategy undergoing clinical evaluation in CRPC is targeting BET family proteins (ClinicalTrials.gov identifier: NCT02711956, NCT03150056). Several BETi, and PROTAC induced BET protein degraders, have shown promising efficacy in preclinical models of CRPC, regulating AR signaling and AR-V7 expression (29,30,(33)(34)(35)(36). Although the mechanism by which BET inhibition regulates AR signaling is well described, the ability to regulate expression of AR-V7…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, increased BRD4 protein stability in substrate-binding adaptor speckle-type POZ protein (SPOP) mutant prostate cancers is associated with AR signaling (31,32). BET inhibitors (BETi) and proteolysis targeting chimera (PROTAC) induced BET protein degraders have anti-tumor activity in CRPC models (29,30,(33)(34)(35)(36), attenuating AR signaling and potently reducing C-MYC expression (29,30,33,34,36). More recently, BETi have been shown to decrease AR-V7 expression by regulating splicing factors required for its generation (30).…”

Section: Introductionmentioning

confidence: 99%

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

Welti

Sharp

Yuan

et al. 2018

Clinical Cancer Research

119

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Welti et al; Targeting BET family proteins in CRPC 2 Statement of Translational RelevanceAdvanced prostate cancer invariably progresses to lethal castration resistant prostate cancer (CRPC). Resistance to current androgen receptor (AR) targeting therapies is associated with the development of AR aberrations including the constitutively active AR splice variant 7 (AR-V7). Currently, no clinically available therapies effectively inhibit aberrant AR signaling. BRD4, a bromodomain and extraterminal (BET) family protein, is a critical AR coregulator. We show that BRD4 expression associates with patient outcome and AR driven transcription in lethal prostate cancer. Moreover, BET inhibitors (BETi) reduce AR splicing and AR-V7 expression by regulating alternative splicing, abrogating AR signaling and inhibiting growth of CRPC patient derived models. Clinical studies with BETi in CRPC should pursue pharmacodynamics studies evaluating abrogation of AR splicing and persistent AR signaling to optimize the development of these drugs for the treatment of CRPC.Research. Experimental Design: We determined associations between BET expression, AR driven transcription and patient outcome; and the effect and mechanism by which chemical BETi (JQ1 and GSK1210151A; I-BET151) and BET family protein knockdown regulates AR-V7 expression and AR signaling in prostate cancer (PC) models.Results: Nuclear BRD4 protein expression increases significantly (p=<0.01) with castration resistance in same patient treatment naïve (median H-score; interquartile range: 100; 100-170) and CRPC (150; 110-200) biopsies, with higher expression at diagnosis associating with worse outcome (HR 3.25, 95% CI 1.50-7.01; p=<0.001). BRD2, BRD3 and BRD4 RNA expression in CRPC biopsies correlates with AR driven transcription (all p=<0.001). Chemical BETi, and combined BET family protein knockdown, reduce AR-V7 expression and AR signaling. This was not recapitulated by C-MYC knockdown. In addition, we show that BETi regulates RNA processing thereby reducing alternative splicing and AR-V7 expression. Furthermore, BETi reduce growth of PC cells and patient derived organoids with known AR mutations, AR amplification and AR-V7 expression. Finally, BETi, unlike enzalutamide, decreases persistent AR signaling and growth (p=<0.001) of a patient derived xenograft model of CRPC with AR amplification and AR-V7 expression. Conclusion:BETi merit clinical evaluation as inhibitors of AR splicing and function, with trials demonstrating their blockade in proof of mechanism pharmacodynamic studies.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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

Welti

Sharp

Yuan

et al. 2018

Clinical Cancer Research

119

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“…Cofactor inhibitors would have the hypothesized advantage that as they are "downstream" of AR, resistance cannot easily be brought about by upregulation of AR or its ligand, making the case for cofactor inhibitor use up-front in combination with traditional antiandrogens to enhance efficacy and block potential resistance mechanisms. Advances in technologies to interrogate chromatin have resulted in the identification of a number of essential AR coactivators and their proposal as potential drug targets (30,(42)(43)(44)(45). Historically, such cofactors and epigenetic regulators have proved notoriously difficult targets for the design of small-molecule inhibitors, hindering progress in this area.…”

Section: Discussionmentioning

confidence: 99%

Therapeutic Targeting of the CBP/p300 Bromodomain Blocks the Growth of Castration-Resistant Prostate Cancer

Jin¹,

Garcia²,

Chan³

et al. 2017

Cancer Research

129

106

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Resistance invariably develops to antiandrogen therapies used to treat newly diagnosed prostate cancers, but effective treatments for castration-resistant disease remain elusive. Here, we report that the transcriptional coactivator CBP/p300 is required to maintain the growth of castration-resistant prostate cancer. To exploit this vulnerability, we developed a novel small-molecule inhibitor of the CBP/p300 bromodomain that blocks prostate cancer growth in vitro and in vivo. Molecular dissection of the consequences of drug treatment revealed a critical role for CBP/p300 in histone acetylation required for the transcriptional activity of the androgen receptor and its target gene expression. Our findings offer a preclinical proof of concept for small-molecule therapies to target the CBP/p300 bromodomain as a strategy to treat castrationresistant prostate cancer. Cancer Res; 77(20); 5564-75. Ó2017 AACR.

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“…Disruption of this interaction with a small-molecule inhibitor of BRD4, JQ1, blocked AR chromatin association, transcriptional activity and AR-mediated PCa growth (Asangani et al 2014). More recently, a pan-BET degrader (based on PROTAC technology) was shown to have potent anti-CRPC activity (Raina et al 2016). Importantly, we and others have shown that BET inhibition has a dual mechanism of action, suppressing not only AR transcriptional activity but also AR gene transcription (Chan et al 2015, Raina et al 2016.…”

Section: Targeting Androgen Receptor Coregulatorsmentioning

confidence: 89%

“…More recently, a pan-BET degrader (based on PROTAC technology) was shown to have potent anti-CRPC activity (Raina et al 2016). Importantly, we and others have shown that BET inhibition has a dual mechanism of action, suppressing not only AR transcriptional activity but also AR gene transcription (Chan et al 2015, Raina et al 2016. This finding, combined with the mapping of the BRD4 interaction surface to the AR-NTD, suggests that BET inhibitors would have activity in CRPC driven by AR-LBD mutants and/or AR-Vs, a prediction that has been experimentally substantiated (Chan et al 2015, Asangani et al 2016, Raina et al 2016.…”

Section: Targeting Androgen Receptor Coregulatorsmentioning

confidence: 99%

Androgen receptor signaling in castration-resistant prostate cancer: a lesson in persistence

Coutinho¹,

Day²,

Tilley³

et al. 2016

Endocrine-Related Cancer

151

122

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The androgen receptor (AR) signaling axis drives all stages of prostate cancer, including the lethal, drug-resistant form of the disease termed castration-resistant prostate cancer (CRPC), which arises after failure of androgen deprivation therapy (ADT). Persistent AR activity in spite of ADT and the second-generation AR-targeting agents enzalutamide and abiraterone is achieved in many cases by direct alterations to the AR signaling axis. Herein, we provide a detailed description of how such alterations contribute to the development and progression of CRPC. Aspects of this broad and ever-evolving field specifically addressed in this review include: the etiology and significance of increased AR expression; the frequency and role of gain-of-function mutations in the AR gene; the function of constitutively active, truncated forms of the AR termed AR variants and the clinical relevance of alterations to the activity and expression of AR coregulators. Additionally, we examine the novel therapeutic strategies to inhibit these classes of therapy resistance mechanisms, with an emphasis on emerging agents that act in a manner distinct from the current ligand-centric approaches. Throughout, we discuss how the central role of AR in prostate cancer and the constant evolution of the AR signaling axis during disease progression represent archetypes of two key concepts in oncology, oncogene addiction and therapy-mediated selection pressure.

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PROTAC-induced BET protein degradation as a therapy for castration-resistant prostate cancer

Cited by 686 publications

References 45 publications

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

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

Therapeutic Targeting of the CBP/p300 Bromodomain Blocks the Growth of Castration-Resistant Prostate Cancer

Androgen receptor signaling in castration-resistant prostate cancer: a lesson in persistence

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