Integrative clinical transcriptome analysis reveals TMPRSS2-ERG dependency of prognostic biomarkers in prostate adenocarcinoma.

6533b82afe1ef96bd128c2a3

RESEARCH PRODUCT

Integrative clinical transcriptome analysis reveals TMPRSS2-ERG dependency of prognostic biomarkers in prostate adenocarcinoma.

Martina Müller-nurasyid Jing Li Thomas G. P. Grunewald Fabienne S. Wehweck Yuri Tolkach Julia S. Gerke Stefanie Stein Giuseppina Sannino Martin F. Orth Tilman L. B. Hoelting Maximilian M. L. Knott Laura Romero-pérez Christian Georg Stief Glen Kristiansen Alexander Buchner Shunya Ohmura Thomas Kirchner Thomas Kirchner Florencia Cidre-aranaz Konstantin Strauch Julian Musa Aruna Marchetto

subject

Oncology Prostate adenocarcinoma Male Cancer Research medicine.medical_specialty Oncogene Proteins Fusion Kaplan-Meier Estimate Adenocarcinoma TMPRSS2 Metastasis Transcriptome 03 medical and health sciences 0302 clinical medicine Internal medicine medicine Biomarkers Tumor Humans Prognostic biomarker Metastasis ; Personalized Medicine ; Prognostic Biomarker ; Prostate Adenocarcinoma ; Tmprss2-erg Neoplasm Metastasis Neoplasm Staging business.industry Gene Expression Profiling Computational Biology Prostatic Neoplasms medicine.disease Prognosis Immunohistochemistry Gene Expression Regulation Neoplastic Oncology 030220 oncology & carcinogenesis Immunohistochemistry Personalized medicine Neoplasm Grading business Erg

description

In prostate adenocarcinoma (PCa), distinction between indolent and aggressive disease is challenging. Around 50% of PCa are characterized by TMPRSS2‐ERG (T2E)‐fusion oncoproteins defining two molecular subtypes (T2E‐positive/negative). However, current prognostic tests do not differ between both molecular subtypes, which might affect outcome prediction. To investigate gene‐signatures associated with metastasis in T2E‐positive and T2E‐negative PCa independently, we integrated tumor transcriptomes and clinicopathological data of two cohorts (total n = 783), and analyzed metastasis‐associated gene‐signatures regarding the T2E‐status. Here, we show that the prognostic value of biomarkers in PCa critically depends on the T2E‐status. Using gene‐set enrichment analyses, we uncovered that metastatic T2E‐positive and T2E‐negative PCa are characterized by distinct gene‐signatures. In addition, by testing genes shared by several functional gene‐signatures for their association with event‐free survival in a validation cohort (n = 272), we identified five genes (ASPN, BGN, COL1A1, RRM2 and TYMS)—three of which are included in commercially available prognostic tests—whose high expression was significantly associated with worse outcome exclusively in T2E‐negative PCa. Among these genes, RRM2 and TYMS were validated by immunohistochemistry in another validation cohort (n = 135), and several of them proved to add prognostic information to current clinicopathological predictors, such as Gleason score, exclusively for T2E‐negative patients. No prognostic biomarkers were identified exclusively for T2E‐positive tumors. Collectively, our study discovers that the T2E‐status, which is per se not a strong prognostic biomarker, crucially determines the prognostic value of other biomarkers. Our data suggest that the molecular subtype needs to be considered when applying prognostic biomarkers for outcome prediction in PCa.

year	journal	country	edition	language
2019-11-29	International journal of cancerReferences

10.1002/ijc.32792 https://pubmed.ncbi.nlm.nih.gov/31732966