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Author Correction: Conservation of copy number profiles during engraftment and passaging of patient-derived cancer xenografts

Authors :
Michael Lloyd
R. Jay Mashl
Yvonne A. Evrard
Jeffrey A. Moscow
Jong Il Kim
Alana L. Welm
Michael A. Davies
Carol J. Bult
Jayamanna Wickramasinghe
Rania El Botty
Dennis A. Dean
Jessica Giordano
Anuj Srivastava
Sandra D. Scherer
Jacqueline Rosains
Christian Frech
Elisabetta Marangoni
Jeffrey H. Chuang
Ryan Jeon
Shunqiang Li
Matthew H. Bailey
Yun-Suhk Suh
Elodie Modave
Yuanxin Xi
Enzo Medico
Li Ding
Livio Trusolino
Adam Lafferty
Vito W. Rebecca
Han-Kwang Yang
Jing Wang
Annette T. Byrne
Xing Yi Woo
Alice C. O’Farrell
Claudio Isella
Li Chen
Brandi N. Davis-Dusenbery
James H. Doroshow
Sherri R. Davies
Diether Lambrechts
Jos Jonkers
Bingliang Fang
Charles Lee
Roebi de Bruijn
Violeta Serra
Jack A. Roth
Rajesh Patidar
Funda Meric-Bernstam
Petra ter Brugge
Andrew V. Kossenkov
Hyun-Soo Kim
Andrea Bertotti
Emilio Cortes-Sanchez
Chieh-Hsiang Yang
Ramaswamy Govindan
Francesco Galimi
Jelena Randjelovic
Zi-Ming Zhao
Bryan E. Welm
Hua Sun
Meenhard Herlyn
Michael T. Lewis
Source :
Nature Genetics
Publication Year :
2021
Publisher :
Springer Science and Business Media LLC, 2021.

Abstract

Patient-derived xenografts (PDXs) are resected human tumors engrafted into mice for preclinical studies and therapeutic testing. It has been proposed that the mouse host affects tumor evolution during PDX engraftment and propagation, affecting the accuracy of PDX modeling of human cancer. Here, we exhaustively analyze copy number alterations (CNAs) in 1,451 PDX and matched patient tumor (PT) samples from 509 PDX models. CNA inferences based on DNA sequencing and microarray data displayed substantially higher resolution and dynamic range than gene expression-based inferences, and they also showed strong CNA conservation from PTs through late-passage PDXs. CNA recurrence analysis of 130 colorectal and breast PT/PDX-early/PDX-late trios confirmed high-resolution CNA retention. We observed no significant enrichment of cancer-related genes in PDX-specific CNAs across models. Moreover, CNA differences between patient and PDX tumors were comparable to variations in multiregion samples within patients. Our study demonstrates the lack of systematic copy number evolution driven by the PDX mouse host.

Details

ISSN :
15461718 and 10614036
Volume :
53
Database :
OpenAIRE
Journal :
Nature Genetics
Accession number :
edsair.doi.dedup.....6d859b9e392055904a93b54d5b1c35a8