Kled: an ultra-fast and sensitive structural variant detection tool for long-read sequencing data

Zhendong Zhang; Tao Jiang; Gaoyang Li; Shuqi Cao; Yadong Liu; Bo Liu; Yadong Wang

doi:10.1093/bib/bbae049

Kled: an ultra-fast and sensitive structural variant detection tool for long-read sequencing data

Brief Bioinform. 2024 Jan 22;25(2):bbae049. doi: 10.1093/bib/bbae049.

Authors

Zhendong Zhang^{1

2}, Tao Jiang^{1

3

2}, Gaoyang Li^{1

2}, Shuqi Cao^{1

2}, Yadong Liu^{1

3

2}, Bo Liu^{1

3

2}, Yadong Wang^{1

3

2}

Affiliations

¹ Center for Bioinformatics, Faculty of Computing, Harbin Institute of Technology, Harbin, Heilongjiang 150001, China.
² Key Laboratory of Biological Bigdata, Ministry of Education, Harbin Institute of Technology, Harbin, Heilongjiang 150001, China.
³ Zhengzhou Research Institute, Harbin Institute of Technology, Zhengzhou, Henan, 450000, China.

Abstract

Structural Variants (SVs) are a crucial type of genetic variant that can significantly impact phenotypes. Therefore, the identification of SVs is an essential part of modern genomic analysis. In this article, we present kled, an ultra-fast and sensitive SV caller for long-read sequencing data given the specially designed approach with a novel signature-merging algorithm, custom refinement strategies and a high-performance program structure. The evaluation results demonstrate that kled can achieve optimal SV calling compared to several state-of-the-art methods on simulated and real long-read data for different platforms and sequencing depths. Furthermore, kled excels at rapid SV calling and can efficiently utilize multiple Central Processing Unit (CPU) cores while maintaining low memory usage. The source code for kled can be obtained from https://github.com/CoREse/kled.

Keywords: long-read sequencing; structural variation; variant calling.

MeSH terms

Algorithms*
Genomics*
Phenotype
Software

Abstract

MeSH terms

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