Patient-derived Models of Abiraterone- and Enzalutamide-resistant Prostate Cancer Reveal Sensitivity to Ribosome-directed Therapy

Mitchell G Lawrence,Daniel Moon,Catherine Mitchell,Daisuke Obinata,Ross D Hannan,John Kourambas,Alisee Huglo,Heather Thorne,Mark Frydenberg,Sam Norden,Luke A Selth,Elena Castro,Shahneen Sandhu,Jeremy Grummet,David Clouston,Birunthi Niranjan,Shivakumar Keerthikumar,Ross Snow,Ashlee K Clark,Jeremy Goad,Yingming Li,Scott M Dehm,Natalie Lister,Luc Furic,Arun Azad,Laurence Harewood,Rendong Yang,Nathan Lawrentschuk,Damien Bolton,David Pook,Wayne D Tilley,Gail P Risbridger,Jenna Van Gramberg,Christine Henzler,Stephen Q Wong,John Pedersen,Melissa Papargiris,Patricia Banks,Shelley Hedwards,Hong Wang,Roxanne Toivanen,Andrew Ryan,Laura H Porter,Richard J Rebello,Adrienne R Hanson,Renea A Taylor,Richard B Pearson,David Goode ,Carmel Pezaro ,Fernando López-Campos ,Declan Murphy ,Shamik Sengupta

doi:10.1016/j.eururo.2018.06.020

Abstract

BackgroundThe intractability of castration-resistant prostate cancer (CRPC) is exacerbated by tumour heterogeneity, including diverse alterations to the androgen receptor (AR) axis and AR-independent phenotypes. The availability of additional models encompassing this heterogeneity would facilitate the identification of more effective therapies for CRPC. ObjectiveTo discover therapeutic strategies by exploiting patient-derived models that exemplify the heterogeneity of CRPC. Design, setting, and participantsFour new patient-derived xenografts (PDXs) were established from independent metastases of two patients and characterised using integrative genomics. A panel of rationally selected drugs was tested using an innovative ex vivo PDX culture system. InterventionThe following drugs were evaluated: AR signalling inhibitors (enzalutamide and galeterone), a PARP inhibitor (talazoparib), a chemotherapeutic (cisplatin), a CDK4/6 inhibitor (ribociclib), bromodomain and extraterminal (BET) protein inhibitors (iBET151 and JQ1), and inhibitors of ribosome biogenesis/function (RNA polymerase I inhibitor CX-5461 and pan-PIM kinase inhibitor CX-6258). Outcome measurements and statistical analysisDrug efficacy in ex vivo cultures of PDX tissues was evaluated using immunohistochemistry for Ki67 and cleaved caspase-3 levels. Candidate drugs were also tested for antitumour efficacy in vivo, with tumour volume being the primary endpoint. Two-tailed t tests were used to compare drug and control treatments. Results and limitationsIntegrative genomics revealed that the new PDXs exhibited heterogeneous mechanisms of resistance, including known and novel AR mutations, genomic structural rearrangements of the AR gene, and a neuroendocrine-like AR-null phenotype. Despite their heterogeneity, all models were sensitive to the combination of ribosome-targeting agents CX-5461 and CX-6258. ConclusionsThis study demonstrates that ribosome-targeting drugs may be effective against diverse CRPC subtypes including AR-null disease, and highlights the potential of contemporary patient-derived models to prioritise treatment strategies for clinical translation. Patient summaryDiverse types of therapy-resistant prostate cancers are sensitive to a new combination of drugs that inhibit protein synthesis pathways in cancer cells.

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