학술논문
Patient-derived xenograft models capture genomic heterogeneity in endometrial cancer
Document Type
article
Author
Vanessa F. Bonazzi; Olga Kondrashova; Deborah Smith; Katia Nones; Asmerom T. Sengal; Robert Ju; Leisl M. Packer; Lambros T. Koufariotis; Stephen H. Kazakoff; Aimee L. Davidson; Priya Ramarao-Milne; Vanessa Lakis; Felicity Newell; Rebecca Rogers; Claire Davies; James Nicklin; Andrea Garrett; Naven Chetty; Lewis Perrin; John V. Pearson; Ann-Marie Patch; Nicola Waddell; Pamela M. Pollock
Source
Genome Medicine, Vol 14, Iss 1, Pp 1-19 (2022)
Subject
Language
English
ISSN
1756-994X
Abstract
Abstract Background Endometrial cancer (EC) is a major gynecological cancer with increasing incidence. It comprises four molecular subtypes with differing etiology, prognoses, and responses to chemotherapy. In the future, clinical trials testing new single agents or combination therapies will be targeted to the molecular subtype most likely to respond. As pre-clinical models that faithfully represent the molecular subtypes of EC are urgently needed, we sought to develop and characterize a panel of novel EC patient-derived xenograft (PDX) models. Methods Here, we report whole exome or whole genome sequencing of 11 PDX models and their matched primary tumor. Analysis of multiple PDX lineages and passages was performed to study tumor heterogeneity across lineages and/or passages. Based on recent reports of frequent defects in the homologous recombination (HR) pathway in EC, we assessed mutational signatures and HR deficiency scores and correlated these with in vivo responses to the PARP inhibitor (PARPi) talazoparib in six PDXs representing the copy number high/p53-mutant and mismatch-repair deficient molecular subtypes of EC. Results PDX models were successfully generated from grade 2/3 tumors, including three uterine carcinosarcomas. The models showed similar histomorphology to the primary tumors and represented all four molecular subtypes of EC, including five mismatch-repair deficient models. The different PDX lineages showed a wide range of inter-tumor and intra-tumor heterogeneity. However, for most PDX models, one arm recapitulated the molecular landscape of the primary tumor without major genomic drift. An in vivo response to talazoparib was detected in four copy number high models. Two models (carcinosarcomas) showed a response consistent with stable disease and two models (one copy number high serous EC and another carcinosarcoma) showed significant tumor growth inhibition, albeit one consistent with progressive disease; however, all lacked the HR deficiency genomic signature. Conclusions EC PDX models represent the four molecular subtypes of disease and can capture intra-tumor heterogeneity of the original primary tumor. PDXs of the copy number high molecular subtype showed sensitivity to PARPi; however, deeper and more durable responses will likely require combination of PARPi with other agents.