Comparison of structural variant callers for massive whole-genome sequence data

Cited 8 time in scopus
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Title
Comparison of structural variant callers for massive whole-genome sequence data
Author(s)
Soobok JoeJong Lyul Park; J Kim; Sangok Kim; Ji Hwan Park; M K Yeo; Dongyoon Lee; Jin Ok YangSeon-Young Kim
Bibliographic Citation
BMC Genomics, vol. 25, pp. 318-318
Publication Year
2024
Abstract
Background: Detecting structural variations (SVs) at the population level using next-generation sequencing (NGS) requires substantial computational resources and processing time. Here, we compared the performances of 11 SV callers: Delly, Manta, GridSS, Wham, Sniffles, Lumpy, SvABA, Canvas, CNVnator, MELT, and INSurVeyor. These SV callers have been recently published and have been widely employed for processing massive whole-genome sequencing datasets. We evaluated the accuracy, sequence depth, running time, and memory usage of the SV callers. Results: Notably, several callers exhibited better calling performance for deletions than for duplications, inversions, and insertions. Among the SV callers, Manta identified deletion SVs with better performance and efficient computing resources, and both Manta and MELT demonstrated relatively good precision regarding calling insertions. We confirmed that the copy number variation callers, Canvas and CNVnator, exhibited better performance in identifying long duplications as they employ the read-depth approach. Finally, we also verified the genotypes inferred from each SV caller using a phased long-read assembly dataset, and Manta showed the highest concordance in terms of the deletions and insertions. Conclusions: Our findings provide a comprehensive understanding of the accuracy and computational efficiency of SV callers, thereby facilitating integrative analysis of SV profiles in diverse large-scale genomic datasets.
Keyword
Large-scale genomic datasetStructural variationWhole-genome sequencing
ISSN
1471-2164
Publisher
Springer-BMC
Full Text Link
http://dx.doi.org/10.1186/s12864-024-10239-9
Type
Article
Appears in Collections:
Aging Convergence Research Center > 1. Journal Articles
Division of A.I. & Biomedical Research > Genomic Medicine Research Center > 1. Journal Articles
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