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    Representation of genomic intratumor heterogeneity in multi-region non-small cell lung cancer patient-derived xenograft models

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    Authors
    Hynds, R. E.
    Huebner, A.
    Pearce, D. R.
    Hil, M. S.
    Akarca, A. U.
    Moore, D. A.
    Ward, S.
    Gowers, K. H. C.
    Karasaki, T.
    Al Bakir, M.
    Wilson, G. A.
    Pich, O.
    Martínez-Ruiz, C.
    Hossain, A S Mukarram
    Pearce, Simon P
    Sivakumar, M.
    Ben Aissa, A.
    Grönroos, E.
    Chandrasekharan, D.
    Kolluri, K. K.
    Towns, R.
    Wang, K. W.
    Cook, D. E.
    Bosshard-Carter, L.
    Naceur-Lombardelli, C.
    Rowan, A. J.
    Veeriah, S.
    Litchfield, K.
    Crosbie, P. A. J.
    Dive, C.
    Quezada, S. A.
    Janes, S. M.
    Jamal-Hanjani, M.
    Marafioti, T.
    McGranahan, N.
    Swanton, C.
    Consortium, T. R.
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    Affiliation
    Cancer Research UK National Biomarker Centre, University of Manchester, Manchester, UK; Cancer Research UK Lung Cancer Centre of Excellence, University of Manchester, Manchester, UK
    Issue Date
    2024
    
    Metadata
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    Abstract
    Patient-derived xenograft (PDX) models are widely used in cancer research. To investigate the genomic fidelity of non-small cell lung cancer PDX models, we established 48 PDX models from 22 patients enrolled in the TRACERx study. Multi-region tumor sampling increased successful PDX engraftment and most models were histologically similar to their parent tumor. Whole-exome sequencing enabled comparison of tumors and PDX models and we provide an adapted mouse reference genome for improved removal of NOD scid gamma (NSG) mouse-derived reads from sequencing data. PDX model establishment caused a genomic bottleneck, with models often representing a single tumor subclone. While distinct tumor subclones were represented in independent models from the same tumor, individual PDX models did not fully recapitulate intratumor heterogeneity. On-going genomic evolution in mice contributed modestly to the genomic distance between tumors and PDX models. Our study highlights the importance of considering primary tumor heterogeneity when using PDX models and emphasizes the benefit of comprehensive tumor sampling. Patient-derived xenografts are important tools for cancer drug development. Here, the authors develop models from 22 non-small cell lung cancer patients. They show genomic differences between models created from different spatial regions of tumours and a bottleneck on model establishment.
    Citation
    Hynds RE, Huebner A, Pearce DR, Hil MS, Akarca AU, Moore DA, et al. Representation of genomic intratumor heterogeneity in multi-region non-small cell lung cancer patient-derived xenograft models. Nature communications. 2024 MAY 31;15(1). PubMed PMID: WOS:001236598600008. English.
    Journal
    Nature Communications
    URI
    http://hdl.handle.net/10541/627031
    DOI
    10.1038/s41467-024-47547-3
    PubMed ID
    38821942
    Additional Links
    https://dx.doi.org/10.1038/s41467-024-47547-3
    Type
    Article
    Language
    en
    ae974a485f413a2113503eed53cd6c53
    10.1038/s41467-024-47547-3
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