Molecular Evolution of Early-Onset Prostate Cancer Identifies Molecular Risk Markers and Clinical Trajectories

早期前列腺癌的分子演化揭示分子风险标志物和临床轨迹

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作者:Clarissa Gerhauser ,Francesco Favero ,Thomas Risch ,Ronald Simon ,Lars Feuerbach ,Yassen Assenov ,Doreen Heckmann ,Nikos Sidiropoulos ,Sebastian M Waszak ,Daniel Hübschmann ,Alfonso Urbanucci ,Etsehiwot G Girma ,Vladimir Kuryshev ,Leszek J Klimczak ,Natalie Saini ,Adrian M Stütz ,Dieter Weichenhan ,Lisa-Marie Böttcher ,Reka Toth ,Josephine D Hendriksen ,Christina Koop ,Pavlo Lutsik ,Sören Matzk ,Hans-Jörg Warnatz ,Vyacheslav Amstislavskiy ,Clarissa Feuerstein ,Benjamin Raeder ,Olga Bogatyrova ,Eva-Maria Schmitz ,Claudia Hube-Magg ,Martina Kluth ,Hartwig Huland ,Markus Graefen ,Chris Lawerenz ,Gervaise H Henry ,Takafumi N Yamaguchi ,Alicia Malewska ,Jan Meiners ,Daniela Schilling ,Eva Reisinger ,Roland Eils ,Matthias Schlesner ,Douglas W Strand ,Robert G Bristow ,Paul C Boutros ,Christof von Kalle ,Dmitry Gordenin ,Holger Sültmann ,Benedikt Brors ,Guido Sauter ,Christoph Plass ,Marie-Laure Yaspo ,Jan O Korbel ,Thorsten Schlomm ,Joachim Weischenfeldt

Abstract

Identifying the earliest somatic changes in prostate cancer can give important insights into tumor evolution and aids in stratifying high- from low-risk disease. We integrated whole genome, transcriptome and methylome analysis of early-onset prostate cancers (diagnosis ≤55 years). Characterization across 292 prostate cancer genomes revealed age-related genomic alterations and a clock-like enzymatic-driven mutational process contributing to the earliest mutations in prostate cancer patients. Our integrative analysis identified four molecular subgroups, including a particularly aggressive subgroup with recurrent duplications associated with increased expression of ESRP1, which we validate in 12,000 tissue microarray tumors. Finally, we combined the patterns of molecular co-occurrence and risk-based subgroup information to deconvolve the molecular and clinical trajectories of prostate cancer from single patient samples.

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