A pathogenic deletion in Forkhead Box L1 (FOXL1) identifies the first otosclerosis (OTSC) gene

Author:

Abdelfatah Nelly,Mostafa Ahmed A.,French Curtis R.,Doucette Lance P.,Penney Cindy,Lucas Matthew B.,Griffin Anne,Booth Valerie,Rowley Christopher,Besaw Jessica E.,Tranebjærg Lisbeth,Rendtorff Nanna Dahl,Hodgkinson Kathy A.,Little Leichelle A.,Agrawal Sumit,Parnes Lorne,Batten Tony,Moore Susan,Hu Pingzhao,Pater Justin A.,Houston Jim,Galutira Dante,Benteau Tammy,MacDonald Courtney,French Danielle,O’Rielly Darren D.,Stanton Susan G.,Young Terry-LynnORCID

Abstract

AbstractOtosclerosis is a bone disorder of the otic capsule and common form of late-onset hearing impairment. Considered a complex disease, little is known about its pathogenesis. Over the past 20 years, ten autosomal dominant loci (OTSC1-10) have been mapped but no genes identified. Herein, we map a new OTSC locus to a 9.96 Mb region within the FOX gene cluster on 16q24.1 and identify a 15 bp coding deletion in Forkhead Box L1 co-segregating with otosclerosis in a Caucasian family. Pre-operative phenotype ranges from moderate to severe hearing loss to profound sensorineural loss requiring a cochlear implant. Mutant FOXL1 is both transcribed and translated and correctly locates to the cell nucleus. However, the deletion of 5 residues in the C-terminus of mutant FOXL1 causes a complete loss of transcriptional activity due to loss of secondary (alpha helix) structure. FOXL1 (rs764026385) was identified in a second unrelated case on a shared background. We conclude that FOXL1 (rs764026385) is pathogenic and causes autosomal dominant otosclerosis and propose a key inhibitory role for wildtype Foxl1 in bone remodelling in the otic capsule. New insights into the molecular pathology of otosclerosis from this study provide molecular targets for non-invasive therapeutic interventions.

Funder

Canadian Institutes of Health Research

Genome Canada

Publisher

Springer Science and Business Media LLC

Subject

Genetics(clinical),Genetics

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