Expression of Androgen Receptor Splice Variants in Prostate Cancer Bone Metastases is Associated with Castration-Resistance and Short Survival

Hörnberg, Emma; Ylitalo, Erik Bovinder; Crnalic, Sead; Antti, Henrik; Stattin, Pär; Widmark, Anders; Bergh, Anders; Wikström, Pernilla

doi:10.1371/journal.pone.0019059

Cited by 415 publications

(525 citation statements)

References 26 publications

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“…This data is also consistent with observations of ARV expression in non-cancerous prostate tissues [10,12,30]. While such low expression of the ARVs challenges their physiological significance, a recent study of prostate cancer bone metastases shows that mRNA levels may not accurately reflect protein levels [18]. We did not assess protein levels of the ARVs identified in the breast cancer cell lines because our primary aim was to examine the frequency and diversity of variant transcript expression.…”

Section: G C T a C T C T T C A G C A T T A G T C C T G T G A A G G Asupporting

confidence: 83%

“…Most ARVs have been shown to be constitutively (AR-V3, -V4, -V7, and -V12) [9,10,12,17] or conditionally (AR-V1 and -V9) [10,12] active androgen-independent transcription factors in a prostate cancer context. Pre-clinical and clinical studies have supported the concept that ARVs are biologically relevant in prostate cancer, particularly in the genesis of a CRPC [11,12,[17][18][19][20].…”

Section: Introductionmentioning

confidence: 97%

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Identification of Androgen Receptor Splice Variant Transcripts in Breast Cancer Cell Lines and Human Tissues

Hickey

Irvine

et al. 2014

HORM CANC

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The androgen receptor (AR) is widely expressed in human tissues and has biological function in many male and female organs. In particular, the AR plays a critical role in the biology and pathology of the prostate gland. AR activity inhibits breast growth and has pleiotropic actions in breast cancer that are subtype-dependent. Expression of AR splice variants (ARVs) and their role in prostate carcinogenesis has been elucidated in recent studies. We hypothesised that ARVs are also expressed in breast cancers and other hormone sensitive tissues. Herein, the expression of five previously identified ARV transcripts with documented transcriptional capacity (AR-V1, -V3, -V4, -V7, and -V9) was examined in 6 breast (MFM223, MDA-MB-453, MDA-MB-231, ZR75

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Section: G C T a C T C T T C A G C A T T A G T C C T G T G A A G G Asupporting

confidence: 83%

Section: Introductionmentioning

confidence: 97%

Identification of Androgen Receptor Splice Variant Transcripts in Breast Cancer Cell Lines and Human Tissues

Hickey

Irvine

et al. 2014

HORM CANC

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“…Although the associations between AR-Vs (mRNA and protein) with clinical parameters and drug resistance are compelling, the relevance of these findings has been called into question by the observation that AR-V expression at the mRNA level may only be approximately 0.03-7% of the full-length transcript in CRPC metastases (Hornberg et al 2011, Robinson et al 2015. However, we believe that this is a poor reason to discount the biological relevance of AR-Vs. First, as full-length AR (AR-FL) expression is increased by approximately an order of magnitude in CRPC compared to hormone-sensitive disease (Hu et al 2009), the aformentioned ratio is misleading in terms of absolute expression.…”

Section: Ar Splice Variantsmentioning

confidence: 94%

“…Rapid, reversible induction of AR-V expression can be achieved by alternative splicing (Watson et al 2010, Hu et al 2012, Gillis et al 2013, Liu et al 2013, Yu et al 2014b, whereas genomic rearrangements within the AR gene can mediate a fully androgen-independent phenotype through a mechanism of switching AR expression from full-length AR to ARv567es (Nyquist et al 2013). AR-V mRNAs have been identified in prostate cancer cell lines, xenografts, mouse models and, most importantly, patient specimens (Dehm et al 2008, Guo et al 2009, Hu et al 2009, Watson et al 2010, Hornberg et al 2011, McGrath et al 2013, Robinson et al 2015 (Table 2). The most recent genomic data, based on the detection of unique exon junctions in RNAseq data, estimates that at least 12 distinct AR-V mRNA species are detectable in primary PCa (Cancer Genome Atlas Research 2015) and 23 in mCRPC (Robinson et al 2015) (for a comprehensive summary of the AR splicing landscape, Supplementary Table 2).…”

Section: Ar Splice Variantsmentioning

confidence: 99%

“…Expression of AR-Vs in clinical samples has provided evidence for clinically relevant functions. For example, AR-V7 is elevated in castrate-resistant vs hormoneresponsive tumor tissues (Guo et al 2009, Hu et al 2009), in CRPC vs benign or localized PCa (McGrath et al 2013) and in CRPC bone metastases compared to benign tissues, primary tumors or hormone-naïve bone metastases (Hornberg et al 2011). Although therapydriven increases in AR-V7 expression could be due to ADT-mediated alterations to AR splicing factors, RNAbinding proteins or miRNAs (Liu et al 2014b, Shi et al 2015, Stockley et al 2015, it must be noted that ligand depletion can result in increased expression of the AR gene due to transcriptional autoregulation (described above) (Cai et al 2011).…”

Section: Ar Splice Variantsmentioning

confidence: 99%

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

Coutinho¹,

Day²,

Tilley³

et al. 2016

Endocrine-Related Cancer

138

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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AR-V7 Protein in Circulating Tumor Cells—The Decider for Therapy?

Montgomery

Plymate

2016

JAMA Oncol

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In this issue of JAMA Oncology, Scher et al 1 present additional evidence that the presence of the constitutively active androgen receptor variant 7 (AR-V7) is a marker for resistance to standard androgen deprivation or second line androgen receptor (AR) targeting agents in men with metastatic prostate cancer. Blood samples were drawn prior to therapy and nucleated cells analyzed for protein expression by immunofluorescence for AR-V7 protein.Results were not used for clinical decision making. Remarkably, no patients with circulating tumor cells (CTCs) positive for AR-V7 protein responded to AR-directed therapy (as defined by a >50% prostate-specific antigen decline), and they had significantly worse progression-free survival and overall survival (OS) compared with patients with AR-V7negative CTCs. These findings are in agreement with those previously reported by Antonorakis et al 2 using a different messenger RNA (mRNA)-based CTC assay. 2 These 2 studies provide compelling evidence that AR-V7-positive CTCs are a predictive biomarker for failure to respond to AR-directed therapy (AR-DT).The studies by Scher et al 1 and Antonorakis et al 2 differ in several respects. First, there was a lower proportion of patients with AR-V7-positive CTCs at each line of therapy using the protein-based assay compared with the mRNAbased assay. Although the patient groups were not entirely identical, this difference in detection may reflect greater sensitivity provided by polymerase chain reaction (PCR) vs antibody detection systems. Second, the issues of specificity of antibodies vs PCR are clearly different. Work has been presented showing that AR-V7 antibodies can react with nonprostate tissue and cell lines such as PC-3, in which no AR-V7 message or N-terminal AR protein can be identified. 3 In the study by Scher et al, AR-V7 immunofluorescence was identified in CTCs that were cytokeratin negative or where other presumed CTCs in the sample were negative for AR N-terminal staining that should detect AR-V7. Although relevant in only a small fraction of the patient samples, appropriate prospective and interinstitutional correlative studies should be done to confirm sensitivity and specificity of the assay before the current test can be applied broadly.The study by Scher et al, 1 as well as those of Welti et al, 3 Antonarakis et al, 4 and Hörnberg et al 5 suggest that AR variant CTCs reflect a different underlying tumor biology associated with a more aggressive form of the disease. In all of these studies, AR-V7 expression in tumor tissues or CTCs was correlated with a significantly shorter OS when compared with those with lower levels of AR-V7 in tissue or when

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Expression of Androgen Receptor Splice Variants in Prostate Cancer Bone Metastases is Associated with Castration-Resistance and Short Survival

Cited by 415 publications

References 26 publications

Identification of Androgen Receptor Splice Variant Transcripts in Breast Cancer Cell Lines and Human Tissues

Identification of Androgen Receptor Splice Variant Transcripts in Breast Cancer Cell Lines and Human Tissues

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

AR-V7 Protein in Circulating Tumor Cells—The Decider for Therapy?

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