Role of the Mitochondrial Mutations, m. 827A > G and the Novel m. 7462C > T, in the Origin of Hearing Loss

UEHARA, Daniela Tiaki; RINCON, Daniel; ABREU-SILVA, Ronaldo Serafim; AURICCHIO, Maria Teresa Balester de Mello; TABITH JR., Alfredo; KOK, Fernando; MINGRONI-NETTO, Regina Celia

Artículos de revistas

Fecha

2010

Registro en:

GENETIC TESTING AND MOLECULAR BIOMARKERS, v.14, n.5, p.611-616, 2010

1945-0265

http://producao.usp.br/handle/BDPI/27495

10.1089/gtmb.2010.0011

http://dx.doi.org/10.1089/gtmb.2010.0011

http://repositorioslatinoamericanos.uchile.cl/handle/2250/1624142

Autor

UEHARA, Daniela Tiaki

RINCON, Daniel

ABREU-SILVA, Ronaldo Serafim

AURICCHIO, Maria Teresa Balester de Mello

TABITH JR., Alfredo

KOK, Fernando

MINGRONI-NETTO, Regina Celia

Institución

Universidade de São Paulo (Brasil)

Resumen

Samples from 30 deaf probands exhibiting features suggestive of syndromic mitochondrial deafness or from families with maternal transmission of deafness were selected for investigation of mutations in the mitochondrial genes MT-RNR1 and MT-TS1. Patients with mutation m. 1555A>G had been previously excluded from this sample. In the MT-RNR1 gene, five probands presented the m. 827A>G sequence variant, of uncertain pathogenicity. This change was also detected in 66 subjects of an unaffected control sample of 306 Brazilian individuals from various ethnic backgrounds. Given its high frequency, we consider it unlikely to have a pathogenic role on hereditary deafness. As to the MT-TS1 gene, one proband presented the previously known pathogenic m. 7472insC mutation and three probands presented a novel variant, m. 7462C>T, which was absent from the same control sample of 306 individuals. Because of its absence in control samples and association with a family history of hearing impairment, we suggest it might be a novel pathogenic mutation.

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