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dc.contributor.author Linch M
dc.contributor.author Goh G
dc.contributor.author Hiley C
dc.contributor.author Shanmugabavan Y
dc.contributor.author McGranahan N
dc.contributor.author Rowan A
dc.contributor.author Wong YNS
dc.contributor.author King H
dc.contributor.author Furness A
dc.contributor.author Freeman A
dc.contributor.author Linares J
dc.contributor.author Akarca A
dc.contributor.author Herrero J
dc.contributor.author Rosenthal R
dc.contributor.author Harder N
dc.contributor.author Schmidt G
dc.contributor.author Wilson GA
dc.contributor.author Birkbak NJ
dc.contributor.author Mitter R
dc.contributor.author Dentro S
dc.contributor.author Cathcart P
dc.contributor.author Arya M
dc.contributor.author Johnston E
dc.contributor.author Scott R
dc.contributor.author Hung M
dc.contributor.author Emberton M
dc.contributor.author Attard G
dc.contributor.author Szállási, Zoltán
dc.contributor.author Punwani S
dc.contributor.author Quezada SA
dc.contributor.author Marafioti T
dc.contributor.author Gerlinger M
dc.contributor.author Ahmed HU
dc.contributor.author Swanton C
dc.date.accessioned 2018-06-22T07:08:55Z
dc.date.available 2018-06-22T07:08:55Z
dc.date.issued 2017
dc.identifier.citation pagination=2472-2480; journalVolume=28; journalIssueNumber=10; journalTitle=ANNALS OF ONCOLOGY;
dc.identifier.uri http://repo.lib.semmelweis.hu//handle/123456789/5072
dc.identifier.uri doi:10.1093/annonc/mdx355
dc.description.abstract Background: Intratumoural heterogeneity (ITH) is well recognised in prostate cancer (PC), but its role in high-risk disease is uncertain. A prospective, single-arm, translational study using targeted multiregion prostate biopsies was carried out to study genomic and T-cell ITH in clinically high-risk PC aiming to identify drivers and potential therapeutic strategies. Patients and methods: Forty-nine men with elevated prostate-specific antigen and multiparametric-magnetic resonance imaging detected PC underwent image-guided multiregion transperineal biopsy. Seventy-nine tumour regions from 25 patients with PC underwent sequencing, analysis of mutations, copy number and neoepitopes combined with tumour infiltrating T-cell subset quantification. Results: We demonstrated extensive somatic nucleotide variation and somatic copy number alteration heterogeneity in high-risk PC. Overall, the mutational burden was low (0.93/Megabase), but two patients had hypermutation, with loss of mismatch repair (MMR) proteins, MSH2 and MSH6. Somatic copy number alteration burden was higher in patients with metastatic hormone-naive PC (mHNPC) than in those with high-risk localised PC (hrlPC), independent of Gleason grade. Mutations were rarely ubiquitous and mutational frequencies were similar for mHNPC and hrlPC patients. Enrichment of focal 3q26.2 and 3q21.3, regions containing putative metastasis drivers, was seen in mHNPC patients. We found evidence of parallel evolution with three separate clones containing activating mutations of beta-catenin in a single patient. We demonstrated extensive intratumoural and intertumoural T-cell heterogeneity and high inflammatory infiltrate in the MMR-deficient (MMRD) patients and the patient with parallel evolution of beta-catenin. Analysis of all patients with activating Wnt/beta-catenin mutations demonstrated a low CD8+/FOXP3+ ratio, a potential surrogate marker of immune evasion. Conclusions: The PROGENY (PROstate cancer GENomic heterogeneitY) study provides a diagnostic platform suitable for studying tumour ITH. Genetic aberrations in clinically high-risk PC are associated with altered patterns of immune infiltrate in tumours. Activating mutations of Wnt/beta-catenin signalling pathway or MMRD could be considered as potential biomarkers for immunomodulation therapies. Clinical Trials.gov Identifier: NCT02022371.
dc.relation.ispartof urn:issn:0923-7534
dc.title Intratumoural evolutionary landscape of high-risk prostate cancer: the PROGENY study of genomic and immune parameters
dc.type Journal Article
dc.date.updated 2018-03-06T12:59:31Z
dc.language.rfc3066 en
dc.identifier.mtmt 3289253
dc.identifier.pubmed 28961847
dc.contributor.department SE/AOK/I/IISZPI/MTA-SE-NAP B Agymetasztázis Kutatócsoport
dc.contributor.institution Semmelweis Egyetem


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