Abstract
BackgroundPatients with newly diagnosed non-metastatic prostate adenocarcinoma are typically classified as at low, intermediate, or high risk of disease progression using blood prostate-specific antigen concentration, tumour T category, and tumour pathological Gleason score. Classification is used to both predict clinical outcome and to inform initial management. However, significant heterogeneity is observed in outcome, particularly within the intermediate risk group, and there is an urgent need for additional markers to more accurately hone risk prediction. Recently developed web-based visualization and analysis tools have facilitated rapid interrogation of large transcriptome datasets, and querying broadly across multiple large datasets should identify predictors that are widely applicable.MethodsWe used camcAPP, cBioPortal, CRN, and NIH NCI GDC Data Portal to data mine publicly available large prostate cancer datasets. A test set of biomarkers was developed by identifying transcripts that had: 1) altered abundance in prostate cancer, 2) altered expression in patients with Gleason score 7 tumours and biochemical recurrence, 3) correlation of expression with time until biochemical recurrence across three datasets (Cambridge, Stockholm, MSKCC). Transcripts that met these criteria were then examined in a validation dataset (TCGA-PRAD) using univariate and multivariable models to predict biochemical recurrence in patients with Gleason score 7 tumours.ResultsTwenty transcripts met the test criteria, and 12 were validated in TCGA-PRAD Gleason score 7 patients. Ten of these transcripts remained prognostic in Gleason score 3 + 4 = 7, a sub-group of Gleason score 7 patients typically considered at a lower risk for poor outcome and often not targeted for aggressive management. All transcripts positively associated with recurrence encode or regulate mitosis and cell cycle-related proteins. The top performer was BUB1, one of four key MIR145-3P microRNA targets upregulated in hormone-sensitive as well as castration-resistant PCa. SRD5A2 converts testosterone to its more active form and was negatively associated with biochemical recurrence.ConclusionsUnbiased mining of large patient datasets identified 12 transcripts that independently predicted disease recurrence risk in Gleason score 7 prostate cancer. The mitosis and cell cycle proteins identified are also implicated in progression to castration-resistant prostate cancer, revealing a pivotal role for loss of cell cycle control in the latter.
Highlights
Patients with newly diagnosed non-metastatic prostate adenocarcinoma are typically classified as at low, intermediate, or high risk of disease progression using blood prostate-specific antigen concentration, tumour T category, and tumour pathological Gleason score
For each of the 1816 genes identified by the above algorithm, the Cambridge (n = 111), Stockholm (n = 92), and MSKCC (n = 140) datasets were interrogated for any correlation between transcript abundance and biochemical recurrence (BCR)-free survival across all Gleason scores
For ANKMY1, higher BCR-free survival was observed in association with lower expression in the Cambridge and MSKCC datasets, but with higher expression in the Stockholm dataset
Summary
Patients with newly diagnosed non-metastatic prostate adenocarcinoma are typically classified as at low, intermediate, or high risk of disease progression using blood prostate-specific antigen concentration, tumour T category, and tumour pathological Gleason score. Prostate cancer (PCa) is the most commonly diagnosed non-skin cancer in men and a leading cause of cancer death [1, 2]. Within 2 years ~ 70% of metastatic PCa becomes resistant to androgen deprivation (castration-resistant PCa [CRPC]), leading, almost invariably, to PCa-specific mortality (reviewed in [9]). Given the heterogeneous outcome in patients diagnosed with localized PCa, risk stratification of newly diagnosed patients with non-metastatic disease at presentation is critical to inform clinical management, and treatment options include observation and one or more of radical prostatectomy, radiotherapy, and androgen deprivation therapy [10, 11]
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