Patient-derived xenografts and organoids model therapy response in prostate cancer

Author:

Karkampouna SofiaORCID,La Manna FedericoORCID,De Filippo Maria R.ORCID,Kiener MirjamORCID,De Menna Marta,Zoni EugenioORCID,Grosjean Joël,Klima Irena,Garofoli Andrea,Bolis Marco,Theurillat Jean-PhilippeORCID,Genitsch Vera,Keller David,Booij Tijmen H.,Stirnimann Christian U.,Eng KennethORCID,Sboner Andrea,Ng Charlotte K. Y.ORCID,Piscuoglio SalvatoreORCID,PC Gray,Spahn Martin,Rubin Mark A.ORCID,Thalmann George N.,Julio Marianna Kruithof-deORCID

Abstract

AbstractTherapy resistance and metastatic processes in prostate cancer (PCa) remain undefined, due to lack of experimental models that mimic different disease stages. We describe a novel androgen-dependent PCa patient-derived xenograft (PDX) model from treatment-naïve, soft tissue metastasis (PNPCa). RNA and whole-exome sequencing of the PDX tissue and organoids confirmed transcriptomic and genomic similarity to primary tumor. PNPCa harboursBRCA2 and CHD1somatic mutations, shows anSPOP/FOXA1-like transcriptomic signature and microsatellite instability, which occurs in 3% of advanced PCa and has never been modelledin vivo. Comparison of the treatment-naïve PNPCa with additional metastatic PDXs (BM18, LAPC9), in a medium-throughput organoid screen of FDA-approved compounds, revealed differential drug sensitivities. Multikinase inhibitors (ponatinib, sunitinib, sorafenib) were broadly effective on all PDX- and patient-derived organoids from advanced cases with acquired resistance to standard-of-care compounds. This proof-of-principle study may provide a preclinical tool to screen drug responses to standard-of-care and newly identified, repurposed compounds.

Publisher

Cold Spring Harbor Laboratory

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