| Literature DB >> 33671976 |
Rosemary Ida Kabahuma1,2, Wolf-Dieter Schubert2, Christiaan Labuschagne3, Denise Yan4, Susan Halloran Blanton4,5, Michael Sean Pepper6, Xue Zhong Liu4,5.
Abstract
MYO7A gene encodes unconventional myosin VIIA, which, when mutated, causes a phenotypic spectrum ranging from recessive hearing loss DFNB2 to deaf-blindness, Usher Type 1B (USH1B). MYO7A mutations are reported in nine DFNB2 families to date, none from sub-Saharan Africa.In DNA, from a cohort of 94 individuals representing 92 families from the Limpopo province of South Africa, eight MYO7A variations were detected among 10 individuals. Family studies identified homozygous and compound heterozygous mutations in 17 individuals out of 32 available family members. Four mutations were novel, p.Gly329Asp, p.Arg373His, p.Tyr1780Ser, and p.Pro2126Leufs*5. Two variations, p.Ser617Pro and p.Thr381Met, previously listed as of uncertain significance (ClinVar), were confirmed to be pathogenic. The identified mutations are predicted to interfere with the conformational properties of myosin VIIA through interruption or abrogation of multiple interactions between the mutant and neighbouring residues. Specifically, p.Pro2126Leufs*5, is predicted to abolish the critical site for the interactions between the tail and the motor domain essential for the autoregulation, leaving a non-functional, unregulated protein that causes hearing loss. We have identified MYO7A as a possible key deafness gene among indigenous sub-Saharan Africans. The spectrum of MYO7A mutations in this South African population points to DFNB2 as a specific entity that may occur in a homozygous or in a compound heterozygous state.Entities:
Keywords: DFNB2; MYO7A gene; South African; compound heterozygous; homozygous; recessive hearing loss; spectrum of MYO7A mutations; sub-Saharan Africa
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Year: 2021 PMID: 33671976 PMCID: PMC7919343 DOI: 10.3390/genes12020274
Source DB: PubMed Journal: Genes (Basel) ISSN: 2073-4425 Impact factor: 4.096