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TRsv: simultaneous detection of tandem repeat variations, structural variations, and short indels using long read sequencing data.


ABSTRACT: Tandem repeat copy number variations (TR-CNVs), structural variations (SVs), and short indels have been responsible for many diseases and traits, but no tools exist to distinguish and detect these variants. In this study, we developed a computational tool, TRsv, to distinguish and detect TR-CNVs, SVs, and short indels using long reads. In evaluation with simulated and real datasets, TRsv outperformed existing tools for detection of TR-CNVs and indels and performed equally well for detection of SVs. We demonstrated genome-wide detection of TR-CNVs, including variants associated with gene expression, disease, and quantitative traits, using 160 long-read whole genome sequencing data and TRsv.

SUBMITTER: Kosugi S 

PROVIDER: S-EPMC12366377 | biostudies-literature | 2025 Aug

REPOSITORIES: biostudies-literature

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TRsv: simultaneous detection of tandem repeat variations, structural variations, and short indels using long read sequencing data.

Kosugi Shunichi S   Terao Chikashi C  

Genome biology 20250820 1


Tandem repeat copy number variations (TR-CNVs), structural variations (SVs), and short indels have been responsible for many diseases and traits, but no tools exist to distinguish and detect these variants. In this study, we developed a computational tool, TRsv, to distinguish and detect TR-CNVs, SVs, and short indels using long reads. In evaluation with simulated and real datasets, TRsv outperformed existing tools for detection of TR-CNVs and indels and performed equally well for detection of S  ...[more]

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