TY - JOUR
T1 - Comprehensive characterization of patient-derived xenograft models of pediatric leukemia
AU - Rogojina, Anna
AU - Klesse, Laura J.
AU - Butler, Erin
AU - Kim, Jiwoong
AU - Zhang, He
AU - Xiao, Xue
AU - Guo, Lei
AU - Zhou, Qinbo
AU - Hartshorne, Taylor
AU - Garcia, Dawn
AU - Weldon, Korri
AU - Holland, Trevor
AU - Bandyopadhyay, Abhik
AU - Prado, Luz Perez
AU - Wang, Shidan
AU - Yang, Donghan M.
AU - Langevan, Anne Marie
AU - Zou, Yi
AU - Grimes, Allison C.
AU - Assanasen, Chatchawin
AU - Gidvani-Diaz, Vinod
AU - Zheng, Siyuan
AU - Lai, Zhao
AU - Chen, Yidong
AU - Xie, Yang
AU - Tomlinson, Gail E.
AU - Skapek, Stephen X.
AU - Kurmasheva, Raushan T.
AU - Houghton, Peter J.
AU - Xu, Lin
N1 - Publisher Copyright:
© 2023 The Authors
PY - 2023/11/17
Y1 - 2023/11/17
N2 - Patient-derived xenografts (PDX) remain valuable models for understanding the biology and for developing novel therapeutics. To expand current PDX models of childhood leukemia, we have developed new PDX models from Hispanic patients, a subgroup with a poorer overall outcome. Of 117 primary leukemia samples obtained, successful engraftment and serial passage in mice were achieved in 82 samples (70%). Hispanic patient samples engrafted at a rate (51/73, 70%) that was similar to non-Hispanic patient samples (31/45, 70%). With a new algorithm to remove mouse contamination in multi-omics datasets including methylation data, we found PDX models faithfully reflected somatic mutations, copy-number alterations, RNA expression, gene fusions, whole-genome methylation patterns, and immunophenotypes found in primary tumor (PT) samples in the first 50 reported here. This cohort of characterized PDX childhood leukemias represents a valuable resource in that germline DNA sequencing has allowed the unambiguous determination of somatic mutations in both PT and PDX.
AB - Patient-derived xenografts (PDX) remain valuable models for understanding the biology and for developing novel therapeutics. To expand current PDX models of childhood leukemia, we have developed new PDX models from Hispanic patients, a subgroup with a poorer overall outcome. Of 117 primary leukemia samples obtained, successful engraftment and serial passage in mice were achieved in 82 samples (70%). Hispanic patient samples engrafted at a rate (51/73, 70%) that was similar to non-Hispanic patient samples (31/45, 70%). With a new algorithm to remove mouse contamination in multi-omics datasets including methylation data, we found PDX models faithfully reflected somatic mutations, copy-number alterations, RNA expression, gene fusions, whole-genome methylation patterns, and immunophenotypes found in primary tumor (PT) samples in the first 50 reported here. This cohort of characterized PDX childhood leukemias represents a valuable resource in that germline DNA sequencing has allowed the unambiguous determination of somatic mutations in both PT and PDX.
KW - Cancer
KW - Omics
KW - Transcriptomics
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U2 - 10.1016/j.isci.2023.108171
DO - 10.1016/j.isci.2023.108171
M3 - Article
C2 - 37915590
AN - SCOPUS:85174399966
SN - 2589-0042
VL - 26
JO - iScience
JF - iScience
IS - 11
M1 - 108171
ER -