Genetic architecture and phenotypic landscape of SLC26A4-related hearing loss.
Keiji HondaAndrew J GriffithPublished in: Human genetics (2021)
Mutations of coding regions and splice sites of SLC26A4 cause Pendred syndrome and nonsyndromic recessive hearing loss DFNB4. SLC26A4 encodes pendrin, a transmembrane exchanger of anions and bases. The mutant SLC26A4 phenotype is characterized by inner ear malformations, including an enlarged vestibular aqueduct (EVA), incomplete cochlear partition type II and modiolar hypoplasia, progressive and fluctuating hearing loss, and vestibular dysfunction. A thyroid iodine organification defect can lead to multinodular goiter and distinguishes Pendred syndrome from DFNB4. Pendred syndrome and DFNB4 are each inherited as an autosomal recessive trait caused by biallelic mutations of SLC26A4 (M2). However, there are some EVA patients with only one detectable mutant allele (M1) of SLC26A4. In most European-Caucasian M1 patients, there is a haplotype that consists of 12 variants upstream of SLC26A4, called CEVA (Caucasian EVA), which acts as a pathogenic recessive allele in trans to mutations affecting the coding regions or splice sites of SLC26A4. This combination of an M1 genotype with the CEVA haplotype is associated with a less severe phenotype than the M2 genotype. The phenotype in EVA patients with no mutant alleles of SLC26A4 (M0) has a very low recurrence probability and is likely to be caused by other factors.
Keyphrases
- hearing loss
- intellectual disability
- case report
- newly diagnosed
- muscular dystrophy
- copy number
- wild type
- genome wide
- multiple sclerosis
- ejection fraction
- autism spectrum disorder
- prognostic factors
- oxidative stress
- magnetic resonance imaging
- computed tomography
- african american
- early onset
- ionic liquid
- magnetic resonance
- single cell
- patient reported
- contrast enhanced