SLC26A4 Phenotypic Variability Influences Intra- and Inter-Familial Diagnosis and Management.

Mohamed Tawalbeh,Dunia Aburizeg, Bayan O Abu Alragheb, Wala Sami Alaqrabawi,Zain Dardas,Luma Srour, Baraah Hatem Altarayra,Ayman A Zayed, Zaid El Omari,Bilal Azab

Genes(2022)

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Abstract
is one of the most common genes causing autosomal recessive non-syndromic sensorineural hearing loss (SNHL). It has been reported to cause Pendred Syndrome (PDS) and DFNB4 which is deafness with enlarged vestibular aqueduct (EVA). However, mutated is not conclusive for having either DFNB4 or PDS. Three unrelated Jordanian families consisting of eight affected individuals with congenital bilateral hearing loss (HL) participated in this study. Whole-exome and Sanger sequencing were performed to investigate the underlying molecular etiology of HL. Further clinical investigations, including laboratory blood workup for the thyroid gland, CT scan for the temporal bone, and thyroid ultrasound were performed. Three disease-causing variants were identified in in the three families, two of which were novel. Two families had a novel pathogenic homozygous splice-site accepter variant (c.165-1G>C), while the third family had compound heterozygous pathogenic variants (c.1446G>A; p.Trp482* and c.304G>A; p.Gly102Arg). Our approach helped in redirecting the diagnosis of several affected members of three different families from non-syndromic HL to syndromic HL. Two of the affected individuals had typical PDS, one had DFNB4, while the rest had atypical PDS. Our work emphasized the intra- and inter-familial variability of -related phenotypes. In addition, we highlighted the variable phenotypic impact of on tailoring a personalized healthcare management.
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Key words
DFNB4,Pendred syndrome,SLC26A4,enlarged vestibular aqueduct,hearing loss,heterogeneity
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