Intratumor Heterogeneity: Novel Approaches for Resolving Genomic Architecture and Clonal Evolution

High-throughput genomic technologies have revealed a remarkably complex portrait of intratumor heterogeneity in cancer and have shown that tumors evolve through a reiterative process of genetic diversification and clonal selection. This discovery has challenged the classical paradigm of clonal domin...

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Bibliographic Details
Published inMolecular cancer research Vol. 15; no. 9; pp. 1127 - 1137
Main Authors Gupta, Ravi G, Somer, Robert A
Format Journal Article
LanguageEnglish
Published United States American Association for Cancer Research Inc 01.09.2017
Subjects
Architecture
Biological evolution
Breast cancer
Cancer
Cell interactions
Clonal Evolution - genetics
Clonal selection
Diagnostic systems
Disease resistance
Epigenetics
Evolution
Gene sequencing
Genetic diversity
Genetic Heterogeneity
Genomes
Genomic instability
Genomics - methods
Genotyping
Heterogeneity
Humans
Metastases
Origins
Phylogeny
Populations
Stability
Tissues
Tumors
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Summary:High-throughput genomic technologies have revealed a remarkably complex portrait of intratumor heterogeneity in cancer and have shown that tumors evolve through a reiterative process of genetic diversification and clonal selection. This discovery has challenged the classical paradigm of clonal dominance and brought attention to subclonal tumor cell populations that contribute to the cancer phenotype. Dynamic evolutionary models may explain how these populations grow within the ecosystem of tissues, including linear, branching, neutral, and punctuated patterns. Recent evidence in breast cancer favors branching and punctuated evolution driven by genome instability as well as nongenetic sources of heterogeneity, such as epigenetic variation, hierarchal tumor cell organization, and subclonal cell-cell interactions. Resolution of the full mutational landscape of tumors could help reconstruct their phylogenetic trees and trace the subclonal origins of therapeutic resistance, relapsed disease, and distant metastases, the major causes of cancer-related mortality. Real-time assessment of the tumor subclonal architecture, however, remains limited by the high rate of errors produced by most genome-wide sequencing methods as well as the practical difficulties associated with serial tumor genotyping in patients. This review focuses on novel approaches to mitigate these challenges using bulk tumor, liquid biopsies, single-cell analysis, and deep sequencing techniques. The origins of intratumor heterogeneity and the clinical, diagnostic, and therapeutic consequences in breast cancer are also explored. .
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ISSN:1541-7786
1557-3125
DOI:10.1158/1541-7786.mcr-17-0070