Genomic profiling of subcutaneous patient-derived xenografts reveals immune constraints on tumor evolution in childhood solid cancer

Author:

He FunanORCID,Bandyopadhyay Abhik M.,Klesse Laura J.ORCID,Rogojina Anna,Chun Sang H.,Butler Erin,Hartshorne TaylorORCID,Holland Trevor,Garcia Dawn,Weldon Korri,Prado Luz-Nereida Perez,Langevin Anne-Marie,Grimes Allison C.,Sugalski Aaron,Shah Shafqat,Assanasen Chatchawin,Lai Zhao,Zou Yi,Kurmashev Dias,Xu LinORCID,Xie Yang,Chen Yidong,Wang XiaojingORCID,Tomlinson Gail E.,Skapek Stephen X.,Houghton Peter J.,Kurmasheva Raushan T.ORCID,Zheng SiyuanORCID

Abstract

AbstractSubcutaneous patient-derived xenografts (PDXs) are an important tool for childhood cancer research. Here, we describe a resource of 68 early passage PDXs established from 65 pediatric solid tumor patients. Through genomic profiling of paired PDXs and patient tumors (PTs), we observe low mutational similarity in about 30% of the PT/PDX pairs. Clonal analysis in these pairs show an aggressive PT minor subclone seeds the major clone in the PDX. We show evidence that this subclone is more immunogenic and is likely suppressed by immune responses in the PT. These results suggest interplay between intratumoral heterogeneity and antitumor immunity may underlie the genetic disparity between PTs and PDXs. We further show that PDXs generally recapitulate PTs in copy number and transcriptomic profiles. Finally, we report a gene fusion LRPAP1-PDGFRA. In summary, we report a childhood cancer PDX resource and our study highlights the role of immune constraints on tumor evolution.

Funder

Cancer Prevention and Research Institute of Texas

U.S. Department of Health & Human Services | NIH | National Cancer Institute

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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