Abstract

Cancer progression in humans is difficult to infer because we do not routinely sample patients at multiple stages of their disease. However, heterogeneous breast tumors provide a unique opportunity to study human tumor progression because they still contain evidence of early and intermediate subpopulations in the form of the phylogenetic relationships. We have developed a method we call Sector-Ploidy-Profiling (SPP) to study the clonal composition of breast tumors. SPP involves macro-dissecting tumors, flow-sorting genomic subpopulations by DNA content, and profiling genomes using comparative genomic hybridization (CGH). Breast carcinomas display two classes of genomic structural variation: (1) monogenomic and (2) polygenomic. Monogenomic tumors appear to contain a single major clonal subpopulation with a highly stable chromosome structure. Polygenomic tumors contain multiple clonal tumor subpopulations, which may occupy the same sectors, or separate anatomic locations. In polygenomic tumors, we show that heterogeneity can be ascribed to a few clonal subpopulations, rather than a series of gradual intermediates. By comparing multiple subpopulations from different anatomic locations, we have inferred pathways of cancer progression and the organization of tumor growth.

Keywords

BiologyComparative genomic hybridizationTumor progressionBreast cancerSomatic evolution in cancerGenomeGenetic heterogeneityChromosomePhylogenetic treeGeneticsPloidyCancerGenePhenotype

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Year
2009
Type
article
Volume
20
Issue
1
Pages
68-80
Citations
522
Access
Closed

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Nicholas E. Navin, Alexander Krasnitz, Linda Rodgers et al. (2009). Inferring tumor progression from genomic heterogeneity. Genome Research , 20 (1) , 68-80. https://doi.org/10.1101/gr.099622.109

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DOI
10.1101/gr.099622.109