| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2042012 | Cell Reports | 2013 | 15 Pages |
•Genome-wide structural variants are highly preserved in breast cancer PDX models•PDXs harbor rarely functionally significant single-nucleotide variants•PDXs harbor ESR1 mutations and translocations associated with endocrine therapy resistance•ESR1 gene amplification in PDX correlated with paradoxical estradiol-induced regression
SummaryTo characterize patient-derived xenografts (PDXs) for functional studies, we made whole-genome comparisons with originating breast cancers representative of the major intrinsic subtypes. Structural and copy number aberrations were found to be retained with high fidelity. However, at the single-nucleotide level, variable numbers of PDX-specific somatic events were documented, although they were only rarely functionally significant. Variant allele frequencies were often preserved in the PDXs, demonstrating that clonal representation can be transplantable. Estrogen-receptor-positive PDXs were associated with ESR1 ligand-binding-domain mutations, gene amplification, or an ESR1/YAP1 translocation. These events produced different endocrine-therapy-response phenotypes in human, cell line, and PDX endocrine-response studies. Hence, deeply sequenced PDX models are an important resource for the search for genome-forward treatment options and capture endocrine-drug-resistance etiologies that are not observed in standard cell lines. The originating tumor genome provides a benchmark for assessing genetic drift and clonal representation after transplantation.
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