Abstract

Glioblastoma (GB) is the most common and aggressive primary brain malignancy, with poor prognosis and a lack of effective therapeutic options. Accumulating evidence suggests that intratumor heterogeneity likely is the key to understanding treatment failure. However, the extent of intratumor heterogeneity as a result of tumor evolution is still poorly understood. To address this, we developed a unique surgical multisampling scheme to collect spatially distinct tumor fragments from 11 GB patients. We present an integrated genomic analysis that uncovers extensive intratumor heterogeneity, with most patients displaying different GB subtypes within the same tumor. Moreover, we reconstructed the phylogeny of the fragments for each patient, identifying copy number alterations in EGFR and CDKN2A/B/p14ARF as early events, and aberrations in PDGFRA and PTEN as later events during cancer progression. We also characterized the clonal organization of each tumor fragment at the single-molecule level, detecting multiple coexisting cell lineages. Our results reveal the genome-wide architecture of intratumor variability in GB across multiple spatial scales and patient-specific patterns of cancer evolution, with consequences for treatment design.

Keywords

CDKN2APTENSomatic evolution in cancerBiologyPDGFRAGenetic heterogeneityCancerMalignancyTumor progressionTumor heterogeneityGlioblastomaComputational biologyEvolutionary biologyCancer researchGeneticsPhenotypeGeneStromal cellPI3K/AKT/mTOR pathway

MeSH Terms

Base SequenceBrain NeoplasmsChromosome AberrationsDNA Copy Number VariationsDNANeoplasmDisease ProgressionEvolutionMolecularGeneserbB-1Genesp16GlioblastomaHumansPhylogenyTranscriptome

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Publication Info

Year
2013
Type
article
Volume
110
Issue
10
Pages
4009-4014
Citations
1690
Access
Closed

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1690
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49
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Cite This

Andrea Sottoriva, Inmaculada Spiteri, Sara Piccirillo et al. (2013). Intratumor heterogeneity in human glioblastoma reflects cancer evolutionary dynamics. Proceedings of the National Academy of Sciences , 110 (10) , 4009-4014. https://doi.org/10.1073/pnas.1219747110

Identifiers

DOI
10.1073/pnas.1219747110
PMID
23412337
PMCID
PMC3593922

Data Quality

Data completeness: 86%