Molecular analysis of SLC26A4 gene in patients with nonsyndromic hearing loss and EVA: identification of two novel mutations in Brazilian patients.

[pendred syndrome]

The SLC 26 A 4 gene has been described as the second gene involved in most cases of sensorineural non-syndromic hearing loss , since the first is the GJB 2 gene . Recessive mutations in the SLC 26 A 4 gene encoding pendrin , an anion transporter , are responsible for non-syndromic hearing loss associated with an enlarged vestibular aqueduct (EVA ) and Pendred syndrome , which causes early hearing loss and affects the thyroid gland . Typically , the hearing loss is profound and prelingual . However , in some individuals , hearing impairment may develop later in childhood and then progress . Over 200 different SLC 26 A 4 mutations have been reported , with each ethnic population having its own distinctive mutant allele series including a few prevalent founder mutations .Perform the screening of the 20 coding exons of SLC 26 A 4 gene in Brazilian deaf individuals with EVA .A mong the 23 unrelated non-syndromic hearing loss Brazilian patients with EVA , in whom no deafness -causing mutations of the GJB 2 gene , the direct sequencing was performed to screen the 20 exons and their flanking regions of the SLC 26 A 4 gene .T he sequencing results revealed 9 cases (39 %) carrying 13 different SLC 26 A 4 mutations , including 11 known mutations (279 delT , V 138 F , T 19 3 I , IVS 8 +1 G >A , T 410 M , Q 413 R , R 409 H , L 445 W , IVS 15 +5 G >A , V 609 G , and R 776 C ) and 2 novel mutation (G 149 R and P 142 L ).The SLC 26 A 4 mutations have a high carrying rate in non-syndromic hearing loss Brazilian patients . The identification of a disease-causing mutation can be used to establish a genotypic diagnosis and provide important information to the patients and their families .