Detection of low prevalence somatic mutations in solid tumors with ultra-deep targeted sequencing

Detection of low prevalence somatic mutations in solid tumors with ultra-deep targeted sequencing

Ultra-deep targeted sequencing (UDT-Seq) can identify subclonal somatic mutations in tumor samples. Early assays' limited breadth and depth restrict their clinical utility. Here, we target 71 kb of mutational hotspots in 42 cancer genes. We present novel methods enhancing both laboratory workfl...

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Veröffentlicht in:Genome Biology (Online Edition) 2011-12, Vol.12 (12), p.R124-R124, Article R124
Hauptverfasser: Harismendy, Olivier, Schwab, Richard B, Bao, Lei, Olson, Jeff, Rozenzhak, Sophie, Kotsopoulos, Steve K, Pond, Stephanie, Crain, Brian, Chee, Mark S, Messer, Karen, Link, Darren R, Frazer, Kelly A
Format: Artikel
Sprache:eng
Schlagworte:
Aged
Animals
Automation, Laboratory
Carcinoma - diagnosis
Carcinoma - genetics
Databases, Genetic
Development and progression
Gene mutations
Genes, Neoplasm - genetics
Genetic aspects
High-Throughput Nucleotide Sequencing - methods
Humans
Method
Mice
Middle Aged
Mutation
Mutation Rate
Nucleotide sequence
Prevalence studies (Epidemiology)
Sarcoma - diagnosis
Sarcoma - genetics
Sensitivity and Specificity
Sequence Analysis, DNA - methods
Tumors
Xenograft Model Antitumor Assays
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Zusammenfassung:Ultra-deep targeted sequencing (UDT-Seq) can identify subclonal somatic mutations in tumor samples. Early assays' limited breadth and depth restrict their clinical utility. Here, we target 71 kb of mutational hotspots in 42 cancer genes. We present novel methods enhancing both laboratory workflow and mutation detection. We evaluate UDT-Seq true sensitivity and specificity (> 94% and > 99%, respectively) for low prevalence mutations in a mixing experiment and demonstrate its utility using six tumor samples. With an improved performance when run on the Illumina Miseq, the UDT-Seq assay is well suited for clinical applications to guide therapy and study clonal selection in heterogeneous samples.
ISSN:1474-760X
1465-6906
1474-760X
1465-6914
DOI:10.1186/gb-2011-12-12-r124