Gene expression profiles define molecular subtypes of prostate cancer bone metastases with different outcomes and morphology traceable back to the primary tumor

Thysell, Elin; Vidman, Linda; Ylitalo, Erik Bovinder; Jernberg, Emma; Crnalic, Sead; Iglesias-Gato, Diego; Flores‐Morales, Amilcar; Stattin, Pär; Egevad, Lars; Widmark, Anders; Rydén, Patrik; Bergh, Anders; Wikström, Pernilla

doi:10.1002/1878-0261.12526

Cited by 18 publications

(48 citation statements)

References 43 publications

(80 reference statements)

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“…Samples of bone metastases were obtained from a series of fresh-frozen biopsies collected from 70 patients with PC operated for metastatic spinal cord compression at Umeå University Hospital (2003–2013). The patient series have been previously described [ 7 , 9 , 12 ] and clinical characteristics of patients included in the current study are summarized in Table 1 . The study also included 12 separate patients with localized PC who were treated with radical prostatectomy at Umeå University Hospital, between 2008 and 2009; mean age for these men was 60 years (range 48–68 years) and mean serum level of prostate specific antigen (PSA) was 11 ng/ml (range 3.5–26 ng/ml).…”

Section: Methodsmentioning

confidence: 99%

“…By exploring the gene expression in clinical samples of PC bone metastases, we have identified transcriptomic as well as proteomic profiles of suggested clinical relevance [ 7 – 12 ]. Specifically, we have identified three molecular subtypes of bone metastases, termed MetA–C, based on the diverged expression of genes related to AR activity, cell cycle activity, and stroma response [ 12 ]. The MetA subtype shows high AR activity in comparison to MetB and C, while MetB shows higher cell cycle activity than the other subtypes.…”

Section: Introductionmentioning

confidence: 99%

“…Accordingly, MetA patients have the best prognosis after ADT, while MetB patients have by far the worst prognosis. Interestingly, the MetA–C subtypes could be intrinsic, as selected features of MetB (low AR activity and high proliferation) were traceable back to the corresponding primary tumors [ 12 ]. In line with this, PC subtypes with characteristics similar to the MetA–C subtypes have been identified by transcriptomic analysis of primary prostate tumors [ 13 , 14 ].…”

Section: Introductionmentioning

confidence: 99%

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A novel DNA methylation signature is associated with androgen receptor activity and patient prognosis in bone metastatic prostate cancer

et al. 2021

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Background Patients with metastatic prostate cancer (PC) are treated with androgen deprivation therapy (ADT) that initially reduces metastasis growth, but after some time lethal castration-resistant PC (CRPC) develops. A better understanding of the tumor biology in bone metastases is needed to guide further treatment developments. Subgroups of PC bone metastases based on transcriptome profiling have been previously identified by our research team, and specifically, heterogeneities related to androgen receptor (AR) activity have been described. Epigenetic alterations during PC progression remain elusive and this study aims to explore promoter gene methylation signatures in relation to gene expression and tumor AR activity. Materials and methods Genome-wide promoter-associated CpG methylation signatures of a total of 94 tumor samples, including paired non-malignant and malignant primary tumor areas originating from radical prostatectomy samples (n = 12), and bone metastasis samples of separate patients with hormone-naive (n = 14), short-term castrated (n = 4) or CRPC (n = 52) disease were analyzed using the Infinium Methylation EPIC arrays, along with gene expression analysis by Illumina Bead Chip arrays (n = 90). AR activity was defined from expression levels of genes associated with canonical AR activity. Results Integrated epigenome and transcriptome analysis identified pronounced hypermethylation in malignant compared to non-malignant areas of localized prostate tumors. Metastases showed an overall hypomethylation in relation to primary PC, including CpGs in the AR promoter accompanied with induction of AR mRNA levels. We identified a Methylation Classifier for Androgen receptor activity (MCA) signature, which separated metastases into two clusters (MCA positive/negative) related to tumor characteristics and patient prognosis. The MCA positive metastases showed low methylation levels of genes associated with canonical AR signaling and patients had a more favorable prognosis after ADT. In contrast, MCA negative patients had low AR activity associated with hypermethylation of AR-associated genes, and a worse prognosis after ADT. Conclusions A promoter methylation signature classifies PC bone metastases into two groups and predicts tumor AR activity and patient prognosis after ADT. The explanation for the methylation diversities observed during PC progression and their biological and clinical relevance need further exploration.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A novel DNA methylation signature is associated with androgen receptor activity and patient prognosis in bone metastatic prostate cancer

et al. 2021

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“…Studies performing genome-wide expression studies (GWAS) within prostate cancer bone metastases from patients who were either untreated or subjected to androgen-deprivation therapy (ADT) have identified three distinct molecular subtypes within bone lesions [ 37 ]. These three subtypes termed MetA-C display unique gene expression profiles.…”

Section: Bone Homeostasis and The Vicious Cyclementioning

confidence: 99%

“…The other molecular subtypes observed classified as MetB and MetC were responsible for 17% and 12% of cases, respectively. MetB bone metastases have alterations in genes associated with DNA damage repair and cell cycle regulation, whilst MetC metastases have enrichment for genes involved in stromal-epithelial cell interactions [ 37 ]. These genetic profiles within bone metastases were observed to correlate with different therapeutic outcomes, in particular, MetB bone metastases had the lowest levels of serum PSA as well as the poorest outcomes following ADT [ 37 ].…”

Section: Bone Homeostasis and The Vicious Cyclementioning

confidence: 99%

Personal Medicine and Bone Metastases: Biomarkers, Micro-RNAs and Bone Metastases

Wood¹,

Brown

2020

Cancers

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Bone metastasis is a major cause of morbidity within solid tumours of the breast, prostate, lung and kidney. Metastasis to the skeleton is associated with a wide range of complications including bone fractures, spinal cord compression, hypercalcaemia and increased bone pain. Improved treatments for bone metastasis, such as the use of anti-bone resorptive bisphosphonate agents, within post-menopausal women have improved disease-free survival; however, these treatments are not without side effects. There is thus a need for biomarkers, which will predict the risk of developing the spread to bone within these cancers. The application of molecular profiling techniques, together with animal model systems and engineered cell-lines has enabled the identification of a series of potential bone-metastasis biomarker molecules predictive of bone metastasis risk. Some of these biomarker candidates have been validated within patient-derived samples providing a step towards clinical utility. Recent developments in multiplex biomarker quantification now enable the simultaneous measurement of up to 96 micro-RNA/protein molecules in a spatially defined manner with single-cell resolution, thus enabling the characterisation of the key molecules active at the sites of pre-metastatic niche formation as well as tumour-stroma signalling. These technologies have considerable potential to inform biomarker discovery. Additionally, a potential future extension of these discoveries could also be the identification of novel drug targets within cancer spread to bone. This chapter summarises recent findings in biomarker discovery within the key bone metastatic cancers (breast, prostate, lung and renal cell carcinoma). Tissue-based and circulating blood-based biomarkers are discussed from the fields of genomics, epigenetic regulation (micro-RNAs) and protein/cell-signalling together with a discussion of the potential future development of these markers towards clinical development.

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Clinical and biological relevance of the transcriptomic‐based prostate cancer metastasis subtypes MetA‐C

et al. 2021

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To improve treatment of metastatic prostate cancer, the biology of metastases needs to be understood. We recently described three subtypes of prostate cancer bone metastases (MetA-C), based on differential gene expression. The aim of this study was to verify the clinical relevance of these subtypes and to explore their biology and relations to genetic drivers. Freshly-frozen metastasis samples were obtained as hormone-naive (n = 17), short-term castrated (n = 21), or castration-resistant (n = 65) from a total of 67 patients. Previously published sequencing data from 573 metastasis samples were also analyzed. Through transcriptome profiling and sample classification based on a set of predefined MetA-C-differentiating genes, we found that most metastases were heterogeneous for the MetA-C subtypes. Overall, MetA was the most common subtype, while MetB was significantly enriched in castration-resistant samples and in liver metastases, and consistently associated with poor prognosis. By gene set enrichment analysis, the phenotype of MetA was described by high androgen response, protein secretion and adipogenesis, MetB by high cell cycle activity and DNA repair, and MetC by epithelial-to-mesenchymal transition and inflammation. The MetB subtype demonstrated single nucleotide variants of RB transcriptional corepressor 1 (RB1) and loss of 21 genes at chromosome 13, including RB1, but provided independent prognostic value to those genetic aberrations. In conclusion, a distinct set of gene transcripts can be used to classify prostate cancer metastases into the subtypes MetA-C. The MetA-C subtypes show diverse biology, organ tropism, and prognosis. The MetA-C classification

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Gene expression profiles define molecular subtypes of prostate cancer bone metastases with different outcomes and morphology traceable back to the primary tumor

Cited by 18 publications

References 43 publications

A novel DNA methylation signature is associated with androgen receptor activity and patient prognosis in bone metastatic prostate cancer

A novel DNA methylation signature is associated with androgen receptor activity and patient prognosis in bone metastatic prostate cancer

Personal Medicine and Bone Metastases: Biomarkers, Micro-RNAs and Bone Metastases

Clinical and biological relevance of the transcriptomic‐based prostate cancer metastasis subtypes MetA‐C

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