Somatic point mutation calling in low cellularity tumors

Somatic point mutation calling in low cellularity tumors

Somatic mutation calling from next-generation sequencing data remains a challenge due to the difficulties of distinguishing true somatic events from artifacts arising from PCR, sequencing errors or mis-mapping. Tumor cellularity or purity, sub-clonality and copy number changes also confound the iden...

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Veröffentlicht in:PloS one 2013-11, Vol.8 (11), p.e74380
Hauptverfasser: Kassahn, Karin S, Holmes, Oliver, Nones, Katia, Patch, Ann-Marie, Miller, David K, Christ, Angelika N, Harliwong, Ivon, Bruxner, Timothy J, Xu, Qinying, Anderson, Matthew, Wood, Scott, Leonard, Conrad, Taylor, Darrin, Newell, Felicity, Song, Sarah, Idrisoglu, Senel, Nourse, Craig, Nourbakhsh, Ehsan, Manning, Suzanne, Wani, Shivangi, Steptoe, Anita, Pajic, Marina, Cowley, Mark J, Pinese, Mark, Chang, David K, Gill, Anthony J, Johns, Amber L, Wu, Jianmin, Wilson, Peter J, Fink, Lynn, Biankin, Andrew V, Waddell, Nicola, Grimmond, Sean M, Pearson, John V
Format: Artikel
Sprache:eng
Schlagworte:
Admixtures
Bioinformatics
Cancer
Computational Biology
Copy number
DNA Copy Number Variations - genetics
Gene mutation
Genetic aspects
Genomes
Genomics
High-Throughput Nucleotide Sequencing - methods
Humans
Medical research
Mutation
Neoplasms - genetics
Neoplasms - pathology
Point mutation
Point Mutation - genetics
Polymerase Chain Reaction - methods
Sequences
Software
Tumors
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Zusammenfassung:Somatic mutation calling from next-generation sequencing data remains a challenge due to the difficulties of distinguishing true somatic events from artifacts arising from PCR, sequencing errors or mis-mapping. Tumor cellularity or purity, sub-clonality and copy number changes also confound the identification of true somatic events against a background of germline variants. We have developed a heuristic strategy and software (http://www.qcmg.org/bioinformatics/qsnp/) for somatic mutation calling in samples with low tumor content and we show the superior sensitivity and precision of our approach using a previously sequenced cell line, a series of tumor/normal admixtures, and 3,253 putative somatic SNVs verified on an orthogonal platform.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0074380