Optical genome mapping unveils hidden structural variants in neurodevelopmental disorders

Author:

Schrauwen IsabelleORCID,Rajendran Yasmin,Acharya Anushree,Öhman Susanna,Arvio Maria,Paetau Ritva,Siren Auli,Avela Kristiina,Granvik Johanna,Leal Suzanne M.,Määttä Tuomo,Kokkonen Hannaleena,Järvelä Irma

Abstract

AbstractWhile short-read sequencing currently dominates genetic research and diagnostics, it frequently falls short of capturing certain structural variants (SVs), which are often implicated in the etiology of neurodevelopmental disorders (NDDs). Optical genome mapping (OGM) is an innovative technique capable of capturing SVs that are undetectable or challenging-to-detect via short-read methods. This study aimed to investigate NDDs using OGM, specifically focusing on cases that remained unsolved after standard exome sequencing. OGM was performed in 47 families using ultra-high molecular weight DNA. Single-molecule maps were assembled de novo, followed by SV and copy number variant calling. We identified 7 variants of interest, of which 5 (10.6%) were classified as likely pathogenic or pathogenic, located in BCL11A, OPHN1, PHF8, SON, and NFIA. We also identified an inversion disrupting NAALADL2, a gene which previously was found to harbor complex rearrangements in two NDD cases. Variants in known NDD genes or candidate variants of interest missed by exome sequencing mainly consisted of larger insertions (> 1kbp), inversions, and deletions/duplications of a low number of exons (1–4 exons). In conclusion, in addition to improving molecular diagnosis in NDDs, this technique may also reveal novel NDD genes which may harbor complex SVs often missed by standard sequencing techniques.

Funder

National Institute of Neurological Disorders and Stroke

National Institute of Child Health and Human Development

Columbia University Sergievsky Center

Publisher

Springer Science and Business Media LLC

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