ROR-γ drives androgen receptor expression and represents a therapeutic target in castration-resistant prostate cancer

Wang, Junjian; Zou, June X.; Xue, Xiaochang; Cai, Demin; Zhang, Yan; Duan, Zhijian; Xiang, Qiuping; Yang, Joy C.; Louie, Maggie C.; Borowsky, Alexander D.; Gao, Allen C.; Evans, Christopher P.; Lam, Kit S.; Xu, Jianzhen; Kung, Hsing Jien; Evans, Ronald M.; Xu, Yong; Chen, Hong Wu

doi:10.1038/nm.4070

Cited by 158 publications

(177 citation statements)

References 68 publications

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“…Therefore, investigation of the mechanism of CRPC is important. A number of potential mechanisms of CRPC have been reported, including: i) AR overexpression; ii) promiscuous binding and activation of mutant AR by alternative ligands, such as estrogen, progesterone, glucocorticoids, bicalutamide, and flutamide; iii) ligand-independent mechanisms of AR activation via crosstalk with serine/threonine kinase 1 (AKT), erb-b2 receptor tyrosine kinase 2 (HER2), and AKT serine/threonine kinase 1 (AKT1) kinases that phosphorylate the AR, and via long non-coding ANTICANCER RESEARCH 37: 125-134 (2017) 130 RNAs that bind to the AR to stimulate transcription of AR target genes; and iv) AR-independent pathways through signal transducer and activator of transcription 3 (STAT3) signaling or up-regulation of anti-apoptotic BCL2, apoptosis regulator (BCL2) (30)(31)(32)(33)(34). In the present study, we revealed that galectin-3 activated PSA transcription and enhanced expression of AR target genes such as KLK3 and TMPRSS2.…”

Section: Effects Of Galectin-3 Expression In Lncap-gal-3 Cells On Cmentioning

confidence: 99%

Galectin-3 Is Implicated in Tumor Progression and Resistance to Anti-androgen Drug Through Regulation of Androgen Receptor Signaling in Prostate Cancer

Dondoo

Fukumori

Daizumoto

et al. 2017

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Section: Effects Of Galectin-3 Expression In Lncap-gal-3 Cells On Cmentioning

confidence: 99%

Galectin-3 Is Implicated in Tumor Progression and Resistance to Anti-androgen Drug Through Regulation of Androgen Receptor Signaling in Prostate Cancer

Dondoo

Fukumori

Daizumoto

et al. 2017

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“…One latest study reveals that AR expression is driven by the upregulation of RORγ in metastatic CRPC [144]. RORγ can controls AR gene expression through its direct binding to AR promoter via exonic ROR-binding element and association with steroid receptor coactivator members (SRCs).…”

Section: Interaction Of Orphan Nrs With Ar Signaling Pathwaymentioning

confidence: 99%

“…RORγ can controls AR gene expression through its direct binding to AR promoter via exonic ROR-binding element and association with steroid receptor coactivator members (SRCs). RORγ-specific agonist can potently inhibit prostatic tumor growth and metastasis in vivo [144]. Androgen exercises opposite roles on TR2 and TR4: represses TR2 [14] and induces TR4 expression [145].…”

Section: Interaction Of Orphan Nrs With Ar Signaling Pathwaymentioning

confidence: 99%

The emerging roles of orphan nuclear receptors in prostate cancer

Cheung

Wang

et al. 2016

Biochimica et Biophysica Acta (BBA) - Reviews on Cancer

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Orphan nuclear receptors are members of the nuclear receptor (NR) superfamily and are so named because their endogenous physiological ligands are either unknown or may not exist. Because of their important regulatory roles in many key physiological processes, dysregulation of signalings controlled by these receptors is associated with many diseases including cancer. Over years, studies of orphan NRs have become an area of great interest because their specific physiological and pathological roles have not been well-defined, and some of them are promising drug targets for diseases. The recently identified synthetic small molecule ligands, acting as agonists or antagonists, to these orphan NRs not only help to understand better their functional roles but also highlight that the signalings mediated by these ligand-independent NRs in diseases could be therapeutically intervened. This review is a summary of the recent advances in elucidating the emerging functional roles of orphan NRs in cancers, especially prostate cancer. In particular, some orphan NRs, RORγ, TR2, TR4, COUP-IFII, ERRα, DAX1 and SHP, exhibit crosstalk or interference with androgen receptor (AR) signaling in either normal or malignant prostatic cells, highlighting their involvement in prostate cancer progression as androgen and AR signaling pathway play critical roles in this process. We also propose that a better understanding of the mechanism of actions of these orphan NRs in prostate gland or prostate cancer could help to evaluate their potential value as therapeutic targets for prostate cancer.

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“…Lentiviral particles were produced in 293T cells after co-transfection of the above lentivirus vectors, psPAX2 and pMD2.G in 10-cm dishes, as described. 55 siRNAs for gene knockdown were purchased from Dharmacon. The siRNA target sequences for KDM4A are as follows: KDM4A#1, GCUGCAGUAUUGAGAUGCUAA; KDM4A#2, GCCUUGGAUCUUUCUGUGAA; Control, CAGUCGCGUUUGCGACUGG.…”

Section: Methodsmentioning

confidence: 99%

Silencing the epigenetic silencer KDM4A for TRAIL and DR5 simultaneous induction and antitumor therapy

Wang

et al. 2016

Cell Death Differ

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Recombinant TRAIL and agonistic antibodies to death receptors (DRs) have been in clinical trial but displayed limited anti-cancer efficacy. Lack of functional DR expression in tumors is a major limiting factor. We report here that chromatin regulator KDM4A/ JMJD2A, not KDM4B, has a pivotal role in silencing tumor cell expression of both TRAIL and its receptor DR5. In TRAIL-sensitive and -resistant cancer cells of lung, breast and prostate, KDM4A small-molecule inhibitor compound-4 (C-4) or gene silencing strongly induces TRAIL and DR5 expression, and causes TRAIL-dependent apoptotic cell death. KDM4A inhibition also strongly sensitizes cells to TRAIL. C-4 alone potently inhibits tumor growth with marked induction of TRAIL and DR5 expression in the treated tumors and effectively sensitizes them to the newly developed TRAIL-inducer ONC201. Mechanistically, C-4 does not appear to act through the Akt-ERK-FOXO3a pathway. Instead, it switches histone modifying enzyme complexes at promoters of TRAIL and DR5 transcriptional activator CHOP gene by dissociating KDM4A and nuclear receptor corepressor (NCoR)-HDAC complex and inducing the recruitment of histone acetylase CBP. Thus, our results reveal KDM4A as a key epigenetic silencer of TRAIL and DR5 in tumors and establish inhibitors of KDM4A as a novel strategy for effectively sensitizing tumors to TRAIL pathway-based therapeutics. 1-5 The binding triggers configurational changes in the receptor trimer and leads to formation of the deathinducing signaling complex (DISC). Depending on cellular context, extrinsic and/or intrinsic pathway of apoptosis is induced with an initial activation of caspase-8 and -10 at DISC and a subsequent activation of the effector caspases such as caspase -3 or -7. The high-tumor cell selectivity and potency in induction of cell death by TRAIL pathway prompted development of therapeutics in the forms of recombinant soluble TRAIL and agonistic TRAIL-R antibodies. 6,7 However, recent clinical trials demonstrated very limited therapeutic benefits. 8,9 Major resistance mechanisms include low expression and/or function of the TRAIL receptors, overexpression of TRAIL decoy receptors (DcRs) and aberrant expression/activation of the anti-apoptotic proteins, such as c-Flip, Bcl-2 family members and IAPs.10,11 Many synthetic or natural agents and cellular pathways have been identified in sensitizing cancer cells to TRAIL.12,13 Given the limited stability and/or bio-distribution of the current TRAIL-based therapies, alternative strategies are being sought to induce tumor cell-endogenous TRAIL expression to block tumor growth. For example, a cell-based screening for TRAIL gene promoter activator identified small-molecule ONC210/TIC10. The subsequent encouraging results of ONC201 from xenograft tumor studies led to its recent entry into clinical efficacy evaluation. 14,15 ONC201 apparently induces TRAIL in cancer cells through inhibition of Akt and ERK kinase signaling and promoting nuclear translocation of Foxo3a. Interestingly, it can also upregulate DR5. ...

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ROR-γ drives androgen receptor expression and represents a therapeutic target in castration-resistant prostate cancer

Cited by 158 publications

References 68 publications

Galectin-3 Is Implicated in Tumor Progression and Resistance to Anti-androgen Drug Through Regulation of Androgen Receptor Signaling in Prostate Cancer

Galectin-3 Is Implicated in Tumor Progression and Resistance to Anti-androgen Drug Through Regulation of Androgen Receptor Signaling in Prostate Cancer

The emerging roles of orphan nuclear receptors in prostate cancer

Silencing the epigenetic silencer KDM4A for TRAIL and DR5 simultaneous induction and antitumor therapy

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