Sage Journals: Discover world-class research

Abstract

Inference of intra-tumor heterogeneity can provide valuable insight into cancer evolution. Somatic mutations detected by sequencing can help estimate the purity of a tumor sample and reconstruct its subclonal composition. Although several methods have been developed to infer intra-tumor heterogeneity, the majority of these tools rely on variant allele frequencies as estimated via ultra-deep sequencing from multiple samples of the same tumor. In practice, obtaining sequencing data from a large number of samples per patient is only feasible in a few cancer types such as liquid tumors, or in rare cases involving solid tumors selected for research. We introduce CTPsingle, which aims at inferring the subclonal composition by using low-coverage sequencing data from a single tumor sample. We show that CTPsingle is able to infer the purity and the clonality of single-sample tumors with high accuracy, even restricted to a coverage depth of ∼30 × .

Get full access to this article

View all access options for this article.

References

Buttrey

S.E.

2005. Calling the lp_solve linear program software from R, S-PLUS and Excel. J. Stat. Softw., 14, 1–13.

Deshwar

A.G.

, Vembu

, Yung

C.K.

, et al. 2015. PhyloWGS: Reconstructing subclonal composition and evolution from whole-genome sequencing of tumors. Genome Biol. 16, 1–20.

El-Kebir

, Oesper

, Acheson-Field

, et al. 2015. Reconstruction of clonal trees and tumor composition from multi-sample sequencing data. Bioinformatics, 31, i62–i70.

Gerlinger

, Rowan

A.J.

, Horswell

, et al. 2012. Intratumor heterogeneity and branched evolution revealed by multiregion sequencing. N. Engl. J. Med., 366, 883–892.

, Roth

, Khattra

, et al. 2014. TITAN: Inference of copy number architectures in clonal cell populations from tumor whole-genome sequence data. Genome Res. 24, 1881–1893.

Hajirasouliha

, Mahmoody

, and Raphael

B.J.

2014. A combinatorial approach for analyzing intra-tumor heterogeneity from high-throughput sequencing data. Bioinformatics, 30, i78–i86.

Jara

, Hanson

, Quintana

, et al. 2011. DPpackage: Bayesian semi- and nonparametric modeling in R. J. Stat. Softw., 40, 1–30.

Jiao

, Vembu

, Deshwar

, et al. 2014. Inferring clonal evolution of tumors from single nucleotide somatic mutations. BMC Bioinformatics, 15, 1–16.

Khursheed

, Kolla

J.N.

, Kotapalli

, et al. 2013. ARID1B, a member of the human SWI/SNF chromatin remodeling complex, exhibits tumour-suppressor activities in pancreatic cancer cell lines. Br. J. Cancer, 108, 2056–2062.

10.

Klose

R.J.

, Yan

, Tothova

, et al. 2007. The retinoblastoma binding protein RBP2 is an H3K4 demethylase. Cell, 128, 889–900.

11.

MacEachern

S.N.

1998. Computational methods for mixture of Dirichlet process models, 23–43. In Dey

D. D.

, Müller

, and Sinha

, eds. Practical Nonparametric and Semiparametric Bayesian Statistics. Springer-Verlag, New York.

12.

Malikic

, McPherson

A.W.

, Donmez

, et al. 2015. Clonality inference in multiple tumor samples using phylogeny. Bioinformatics, 31, 1349–1356.

13.

Oesper

, Satas

, and Raphael

B.J.

2014. Quantifying tumor heterogeneity in whole-genome and whole-exome sequencing data. Bioinformatics, 30, 3532–3540.

14.

Popic

, Salari

, Hajirasouliha

, et al. 2015. Fast and scalable inference of multi-sample cancer lineages. Genome Biol. 16, 1–17.

15.

Prandi

, Baca

S.C.

, Romanel

, et al. 2014. Unraveling the clonal hierarchy of somatic genomic aberrations. Genome Biol. 15, 1–16.

16.

Roth

, Khattra

, Yap

, et al. 2014. PyClone: Statistical inference of clonal population structure in cancer. Nat. Methods, 11, 396–398.

17.

Schuh

, Becq

, Humphray

, et al. 2012. Monitoring chronic lymphocytic leukemia progression by whole genome sequencing reveals heterogeneous clonal evolution patterns. Blood, 120, 4191–4196.

18.

Sengupta

, Wang

, Lee

, et al. 2015. Bayclone: Bayesian nonparametric inference of tumor subclones using NGS data, 467–478. In Altman

R.B.

, Dunker

A.K.

, Hunter

, et al., eds. Pacific Symposium on Biocomputing 2015. World Scientific Publishing Co. Pte. Ltd., Singapore.

19.

Strino

, Parisi

, Micsinai

, et al. 2013. TrAp: A tree approach for finger-printing subclonal tumor composition. Nucleic Acids Res. 41, e165.

20.

Weinstein

J.N.

, Collisson

E.A.

, Mills

G.B.

, et al. 2013. The cancer genome atlas pan-cancer analysis project. Nat. Genet., 45, 1113–1120.

21.

Zare

, Wang

, Hu

, et al. 2014. Inferring clonal composition from multiple sections of a breast cancer. PLoS Comput. Biol. 10, e1003703.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.52 MB

Clonality Inference from Single Tumor Samples Using Low-Coverage Sequence Data

Abstract

Abstract

Get full access to this article

References

Supplementary Material