A general framework for analyzing tumor subclonality using SNP array and DNA sequencing data

Bo Li; Jun Z. Li

doi:10.1186/s13059-014-0473-4

A general framework for analyzing tumor subclonality using SNP array and DNA sequencing data

Bo Li, Jun Z. Li

Research output: Contribution to journal › Article › peer-review

59 Scopus citations

Abstract

Intra-tumor heterogeneity reflects cancer genome evolution and provides key information for diagnosis and treatment. When bulk tumor tissues are profiled for somatic copy number alterations (sCNA) and point mutations, it may be difficult to estimate their cellular fractions when a mutation falls within a sCNA. We present the Clonal Heterogeneity Analysis Tool, which estimates cellular fractions for both sCNAs and mutations, and uses their distributions to inform macroscopic clonal architecture. In a set of approximately 700 breast tumors, more than half appear to contain multiple recognizable aneuploid tumor clones, and many show subtype-specific differences in clonality for known cancer genes.

Original language	English (US)
Article number	473
Pages (from-to)	473
Number of pages	1
Journal	Genome biology
Volume	15
Issue number	9
DOIs	https://doi.org/10.1186/s13059-014-0473-4
State	Published - 2014

ASJC Scopus subject areas

Ecology, Evolution, Behavior and Systematics
Genetics
Cell Biology

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10.1186/s13059-014-0473-4

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title = "A general framework for analyzing tumor subclonality using SNP array and DNA sequencing data",

abstract = "Intra-tumor heterogeneity reflects cancer genome evolution and provides key information for diagnosis and treatment. When bulk tumor tissues are profiled for somatic copy number alterations (sCNA) and point mutations, it may be difficult to estimate their cellular fractions when a mutation falls within a sCNA. We present the Clonal Heterogeneity Analysis Tool, which estimates cellular fractions for both sCNAs and mutations, and uses their distributions to inform macroscopic clonal architecture. In a set of approximately 700 breast tumors, more than half appear to contain multiple recognizable aneuploid tumor clones, and many show subtype-specific differences in clonality for known cancer genes. ",

author = "Bo Li and Li, {Jun Z.}",

note = "Funding Information: The results presented here are in part based upon data generated by the TCGA Research Network: http://cancergenome.nih.gov/. We would like to thank a Rackham Predoctoral Fellowship (BL) and a Pilot Grant from the Center of Computation Biology and Medicine at University of Michigan (JL) for supporting this research. We thank Drs. Nancy Zhang, Kerby Shedden, and Sebastian Zoellner for helpful discussions.",

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N2 - Intra-tumor heterogeneity reflects cancer genome evolution and provides key information for diagnosis and treatment. When bulk tumor tissues are profiled for somatic copy number alterations (sCNA) and point mutations, it may be difficult to estimate their cellular fractions when a mutation falls within a sCNA. We present the Clonal Heterogeneity Analysis Tool, which estimates cellular fractions for both sCNAs and mutations, and uses their distributions to inform macroscopic clonal architecture. In a set of approximately 700 breast tumors, more than half appear to contain multiple recognizable aneuploid tumor clones, and many show subtype-specific differences in clonality for known cancer genes.

AB - Intra-tumor heterogeneity reflects cancer genome evolution and provides key information for diagnosis and treatment. When bulk tumor tissues are profiled for somatic copy number alterations (sCNA) and point mutations, it may be difficult to estimate their cellular fractions when a mutation falls within a sCNA. We present the Clonal Heterogeneity Analysis Tool, which estimates cellular fractions for both sCNAs and mutations, and uses their distributions to inform macroscopic clonal architecture. In a set of approximately 700 breast tumors, more than half appear to contain multiple recognizable aneuploid tumor clones, and many show subtype-specific differences in clonality for known cancer genes.

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A general framework for analyzing tumor subclonality using SNP array and DNA sequencing data

Abstract

ASJC Scopus subject areas

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