| Literature DB >> 33169910 |
Aboulfazl Rad1, Thore Schade-Mann1, Philipp Gamerdinger1, Grigoriy A Yanus2,3, Björn Schulte4, Marcus Müller1, Evgeny N Imyanitov2,3,5, Saskia Biskup4, Hubert Löwenheim1, Anke Tropitzsch1, Barbara Vona1.
Abstract
Alpha-chain collagen molecules encoded by genes that include COL11A1 are essential for skeletal, ocular, and auditory function. COL11A1 variants have been reported in syndromes involving these organ systems. However, a description of the complete clinical spectrum is lacking, as evidenced by a recent association of autosomal dominant nonsyndromic hearing loss due to a splice-altering variant in COL11A1, mapping the DFNA37 locus. Here, we describe two German families presenting prelingual autosomal dominant nonsyndromic hearing loss with novel COL11A1 heterozygous splice-altering variants (c.652-1G>C and c.4338+2T>C) that were molecularly characterized. Interestingly, the c.652-1G>C variant affects the same intron 4 canonical splice site originally reported in the DFNA37 family (c.652-2A>C) but elicits a different splicing outcome. Furthermore, the c.4338+2T>C variant originated de novo. We provide clinical and molecular genetic evidence to unambiguously confirm that COL11A1 splice-altering variants cause DFNA37 hearing loss and affirm that COL11A1 be included in the genetic testing of patients with nonsyndromic deafness.Entities:
Keywords: COL11A1; DFNA37; autosomal dominant hearing loss; nonsyndromic hearing loss; splice-site altering variant
Mesh:
Substances:
Year: 2020 PMID: 33169910 DOI: 10.1002/humu.24136
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878