DR-444 Characterisation and in-depth analysis of the genome, transcriptome and clinical correlates of metastatic prostate cancer patients for identifying potential druggable targets

In this project we aim to use whole genome and whole transcriptome sequencing data to identify druggable targets for novel and existing drugs, with a focus on antibody drug conjugates and T-cell engagers. Genomics and transcriptomics data will be used to identify genetic subgroups. The presence of druggable targets in both the tumor and its microenvironment will be studied.

John Martens, Erasmus MC, The Netherlands