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Prostate Cancer Heterogeneity: Discovering Novel Molecular Targets for Therapy

Overview
Journal Cancer Treat Rev
Publisher Elsevier
Specialty Oncology
Date 2017 Feb 24
PMID 28231559
Citations 43
Authors
Chiara Ciccarese
Francesco Massari
Roberto Iacovelli
Michelangelo Fiorentino
Rodolfo Montironi
Vincenzo Di Nunno
Francesca Giunchi
Matteo Brunelli
Giampaolo Tortora
Affiliations
Soon will be listed here.
Abstract

Prostate cancer (PCa) shows a broad spectrum of biological and clinical behavior, which represents the epiphenomenon of an extreme genetic heterogeneity. Recent genomic profiling studies have deeply improved the knowledge of the genomic landscape of localized and metastatic PCa. The AR and PI3K/Akt/mTOR signaling pathways are the two most frequently altered, representing therefore interestingly targets for therapy. Moreover, somatic or germline aberrations of DNA repair genes (DRGs) have been observed at high frequency, supporting the potential role of platinum derivatives and PARP inhibitors as effective therapeutic strategies. In the future, the identification of driver mutations present at a specific stage of the disease, the classification PCa based on specific molecular alterations, and the selection of the most appropriate therapy based on biomarkers predictors of response represent the foundations for an increasingly more accurate personalized medicine.

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