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Cited 9 time in webofscience Cited 10 time in scopus
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DeviCNV: detection and visualization of exon-level copy number variants in targeted next-generation sequencing dataopen access

Authors
Kang, Y[Kang, Yeeok]Nam, SH[Nam, Seong-Hyeuk]Park, KS[Park, Kyung Sun]Kim, Y[Kim, Yoonjung]Kim, JW[Kim, Jong-Won]Lee, E[Lee, Eunjung]Ko, JM[Ko, Jung Min]Lee, KA[Lee, Kyung-A]Park, I[Park, Inho]
Issue Date
Oct-2018
Publisher
BMC
Keywords
Copy-number variation; Targeted sequencing; Visualization; Germ-line; Exon-level
Citation
BMC BIOINFORMATICS, v.19, no.1
Indexed
SCIE
SCOPUS
Journal Title
BMC BIOINFORMATICS
Volume
19
Number
1
URI
https://scholarworks.bwise.kr/skku/handle/2021.sw.skku/18112
DOI
10.1186/s12859-018-2409-6
ISSN
1471-2105
Abstract
BackgroundTargeted next-generation sequencing (NGS) is increasingly being adopted in clinical laboratories for genomic diagnostic tests.ResultsWe developed a new computational method, DeviCNV, intended for the detection of exon-level copy number variants (CNVs) in targeted NGS data. DeviCNV builds linear regression models with bootstrapping for every probe to capture the relationship between read depth of an individual probe and the median of read depth values of all probes in the sample. From the regression models, it estimates the read depth ratio of the observed and predicted read depth with confidence interval for each probe which is applied to a circular binary segmentation (CBS) algorithm to obtain CNV candidates. Then, it assigns confidence scores to those candidates based on the reliability and strength of the CNV signals inferred from the read depth ratios of the probes within them. Finally, it also provides gene-centric plots with confidence levels of CNV candidates for visual inspection. We applied DeviCNV to targeted NGS data generated for newborn screening and demonstrated its ability to detect novel pathogenic CNVs from clinical samples.ConclusionsWe propose a new pragmatic method for detecting CNVs in targeted NGS data with an intuitive visualization and a systematic method to assign confidence scores for candidate CNVs. Since DeviCNV was developed for use in clinical diagnosis, sensitivity is increased by the detection of exon-level CNVs.
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