Haplotype-resolved inversion landscape reveals hotspots of mutational recurrence associated with genomic disorders

Author:

Porubsky DavidORCID,Höps WolframORCID,Ashraf Hufsah,Hsieh PingHsunORCID,Rodriguez-Martin BernardoORCID,Yilmaz FeyzaORCID,Ebler JanaORCID,Hallast PilleORCID,Maria Maggiolini Flavia AngelaORCID,Harvey William T.ORCID,Henning BarbaraORCID,Audano Peter A.ORCID,Gordon David S.ORCID,Ebert PeterORCID,Hasenfeld PatrickORCID,Benito EvaORCID,Zhu QihuiORCID,Lee CharlesORCID,Antonacci FrancescaORCID,Steinrücken Matthias,Beck Christine R.ORCID,Sanders Ashley D.ORCID,Marschall TobiasORCID,Eichler Evan E.ORCID,Korbel Jan O.ORCID,

Abstract

AbstractUnlike copy number variants (CNVs), inversions remain an underexplored genetic variation class. By integrating multiple genomic technologies, we discover 729 inversions in 41 human genomes. Approximately 85% of inversions <2 kbp form by twin-priming during L1-retrotransposition; 80% of the larger inversions are balanced and affect twice as many base pairs as CNVs. Balanced inversions show an excess of common variants, and 72% are flanked by segmental duplications (SDs) or mobile elements. Since this suggests recurrence due to non-allelic homologous recombination, we developed complementary approaches to identify recurrent inversion formation. We describe 40 recurrent inversions encompassing 0.6% of the genome, showing inversion rates up to 2.7×10-4 per locus and generation. Recurrent inversions exhibit a sex- chromosomal bias, and significantly co-localize to the critical regions of genomic disorders. We propose that inversion recurrence results in an elevated number of heterozygous carriers and structural SD diversity, which increases mutability in the population and predisposes to disease- causing CNVs.

Publisher

Cold Spring Harbor Laboratory

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