ClinVar

In 8 deaf and 7 hearing members of a large consanguineous Pakistani family (PK2) with prelingual severe-to-profound nonsyndromic hearing loss (DFNM26; 605428), originally studied by Riazuddin et al. (2000), Yousaf et al. (2018) identified homozygosity for a c.347G-A transition (c.347G-A, NM_207123) in exon 2 of the GAB1 gene, resulting in a gly116-to-glu (G116E) substitution at a highly conserved residue within the PH domain. The G116E variant was not found in 380 Pakistani and 192 Indian control chromosomes, or in the 1000 Genomes Project, NHLBI Exome Variant Server, or ExAC databases. Functional analysis of the lipid-binding function of the mutant GAB1 PH domain showed significantly lower amounts bound to phosphoinositides compared to the wildtype PH domain. In addition, phenotypes of gab1-null morphant zebrafish were partially rescued by coinjection of G116E mutant mRNA compared to wildtype GAB1, suggesting that G116E represents a hypomorphic allele. Nonpenetrant hearing members of the family were also heterozygous for a missense mutation in the METTL13 gene (617987.0001), which was not present in any of the deaf members of the family.