Identifying aggressive prostate cancer foci using a DNA methylation classifier

Slow-growing prostate cancer (PC) can be aggressive in a subset of cases. Therefore, prognostic tools to guide clinical decision-making and avoid overtreatment of indolent PC and undertreatment of aggressive disease are urgently needed. PC has a propensity to be multifocal with several different can...

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Bibliographic Details
Published in:Genome Biology 2017-01, Vol.18 (1), p.3-3, Article 3
Main Authors: Mundbjerg, Kamilla, Chopra, Sameer, Alemozaffar, Mehrdad, Duymich, Christopher, Lakshminarasimhan, Ranjani, Nichols, Peter W, Aron, Manju, Siegmund, Kimberly D, Ukimura, Osamu, Aron, Monish, Stern, Mariana, Gill, Parkash, Carpten, John D, Ørntoft, Torben F, Sørensen, Karina D, Weisenberger, Daniel J, Jones, Peter A, Duddalwar, Vinay, Gill, Inderbir, Liang, Gangning
Format: Article
Language:English
Subjects:
aggression
Biomarkers, Tumor
Biopsy
Cluster Analysis
Decision making
Disease Progression
DNA Methylation
DNA probes
early diagnosis
Epigenesis, Genetic
Epigenomics - methods
Gene Expression Profiling
Humans
Invasiveness
Lymph nodes
Lymphatic Metastasis
Male
Metastases
metastasis
monitoring
Neoplasm Metastasis
Neoplasm Staging
patients
Prognosis
Prostate cancer
prostatic neoplasms
Prostatic Neoplasms - genetics
Prostatic Neoplasms - pathology
Prostatic Neoplasms - surgery
Quantitative Trait Loci
Reproducibility of Results
Transcriptome
Tumor Burden
Tumors
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Summary:Slow-growing prostate cancer (PC) can be aggressive in a subset of cases. Therefore, prognostic tools to guide clinical decision-making and avoid overtreatment of indolent PC and undertreatment of aggressive disease are urgently needed. PC has a propensity to be multifocal with several different cancerous foci per gland. Here, we have taken advantage of the multifocal propensity of PC and categorized aggressiveness of individual PC foci based on DNA methylation patterns in primary PC foci and matched lymph node metastases. In a set of 14 patients, we demonstrate that over half of the cases have multiple epigenetically distinct subclones and determine the primary subclone from which the metastatic lesion(s) originated. Furthermore, we develop an aggressiveness classifier consisting of 25 DNA methylation probes to determine aggressive and non-aggressive subclones. Upon validation of the classifier in an independent cohort, the predicted aggressive tumors are significantly associated with the presence of lymph node metastases and invasive tumor stages. Overall, this study provides molecular-based support for determining PC aggressiveness with the potential to impact clinical decision-making, such as targeted biopsy approaches for early diagnosis and active surveillance, in addition to focal therapy.
ISSN:1474-760X
1474-7596
1474-760X
DOI:10.1186/s13059-016-1129-3