Enhanced detection and genotyping of disease-associated tandem repeats using HMMSTR and targeted long-read sequencing

Tandem repeat sequences comprise approximately 8% of the human genome and are linked to more than 50 neurodegenerative disorders. Accurate characterization of disease-associated repeat loci remains resource intensive and often lacks high resolution genotype calls. We introduce a multiplexed, targete...

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Veröffentlicht in:Nucleic acids research 2024-12, Vol.53 (2)
Hauptverfasser: Van Deynze, Kinsey, Mumm, Camille, Maltby, Connor J, Switzenberg, Jessica A, Todd, Peter K, Boyle, Alan P
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Sprache:eng
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Zusammenfassung:Tandem repeat sequences comprise approximately 8% of the human genome and are linked to more than 50 neurodegenerative disorders. Accurate characterization of disease-associated repeat loci remains resource intensive and often lacks high resolution genotype calls. We introduce a multiplexed, targeted nanopore sequencing panel and HMMSTR, a sequence-based tandem repeat copy number caller which outperforms current signal- and sequence-based callers relative to two assemblies and we show it performs with high accuracy in heterozygous regions and at low read coverage. The flexible panel allows us to capture disease associated regions at an average coverage of >150x. Using these tools, we successfully characterize known or suspected repeat expansions in patient derived samples. In these samples, we also identify unexpected expanded alleles at tandem repeat loci not previously associated with the underlying diagnosis. This genotyping approach for tandem repeat expansions is scalable, simple, flexible and accurate, offering significant potential for diagnostic applications and investigation of expansion co-occurrence in neurodegenerative disorders.
ISSN:0305-1048
1362-4962
1362-4962
DOI:10.1093/nar/gkae1202