Aberrant transcript produced by a splice donor site deletion in the TECTA gene is associated with autosomal dominant deafness in a Brazilian family

Karina Lezirovitz; Ana C Batissoco; Fernanda T Lima; Maria T B M Auricchio; Renata W Nonose; Simone R dos Santos; Luiza Guilherme; Jeanne Oiticica; Regina C Mingroni-Netto

doi:10.1016/j.gene.2012.09.023

Aberrant transcript produced by a splice donor site deletion in the TECTA gene is associated with autosomal dominant deafness in a Brazilian family

Gene. 2012 Dec 15;511(2):280-4. doi: 10.1016/j.gene.2012.09.023. Epub 2012 Sep 17.

Authors

Karina Lezirovitz¹, Ana C Batissoco, Fernanda T Lima, Maria T B M Auricchio, Renata W Nonose, Simone R dos Santos, Luiza Guilherme, Jeanne Oiticica, Regina C Mingroni-Netto

Affiliation

¹ Human Genome Research Center, Department of Genetics and Evolutionary Biology, Biosciences Institute, University of São Paulo, São Paulo (SP), Brazil. lezi.karina@gmail.com

PMID: 22995349
DOI: 10.1016/j.gene.2012.09.023

Abstract

We ascertained a Brazilian family with nine individuals affected by autosomal dominant nonsyndromic sensorineural hearing loss. The bilateral hearing loss affected mainly mid-high frequencies, was apparently stable with an early onset. Microsatellites close to the DFNA8/DFNA12 locus, which harbors the TECTA gene, showed significant multipoint lod scores (3.2) close to marker D11S4107. Sequencing of the exons and exon-intron boundaries of the TECTA gene in one affected subject revealed the deletion c.5383+5delGTGA in the 5' end of intron 16, that includes the last two bases of the donor splice site consensus sequence. This mutation segregates with deafness within the family. To date, 33 different TECTA mutations associated with autossomal dominant hearing loss have been described. Among them is the mutation reported herein, first described by Hildebrand et al. (2011) in a UK family. The audioprofiles from the UK and Brazilian families were similar. In order to investigate the transcripts produced by the mutated allele, we performed cDNA analysis of a lymphoblastoid cell line from an affected heterozygote with the c.5383+5delGTGA and a noncarrier from the same family. The analysis allowed us to identify an aberrant transcript with skipping of exon 16, without affecting the reading frame. One of the dominant TECTA mutations already described, a synonymous substitution in exon 16 (c.5331G<A), was also shown to affect splicing, resulting in an aberrant transcript lacking exon 16. Despite the difference in the DNA level, both the synonymous substitution in exon 16 (c.5331G<A) and the mutation described herein affect splicing of exon 16, leading to its skipping. At the protein level they would have the same effect, an in-frame deletion of 37 amino-acids (p.S1758Y/G1759_N1795del) probably leading to an impaired function of the ZP domain. Thus, like the TECTA missense mutations associated with dominant hearing loss, the c.5383+5delGTGA mutation does not have an inactivating effect on the protein.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Base Sequence
Brazil
DNA Primers
Deafness / genetics*
Extracellular Matrix Proteins / genetics*
Female
GPI-Linked Proteins / genetics
Genes, Dominant*
Genetic Linkage
Humans
Male
Pedigree
RNA, Messenger / genetics*

Substances

DNA Primers
Extracellular Matrix Proteins
GPI-Linked Proteins
RNA, Messenger
TECTA protein, human