Audiological profiles and gjb2, gjb6 mutations: A retrospective study on genetic and clinical data from 2003 to 2008

Audiological medicine Pub Date : 2009-01-01 DOI:10.1080/16513860902900136

A. Berto, D. Pellati, A. Castiglione, M. Busi, P. Trevisi, F. Gualandi, A. Ferlini, A. Martini

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引用次数: 8

Abstract

In many world populations, mutations in the GJB2 gene (codifying for Connexin 26) are the most common causes of autosomal recessive non-syndromic hearing loss and account for approximately 50% of cases. To date, more than 100 (dominant or recessive) mutations have been identified (The Connexin Deafness Homepage, 2009) and differences in frequency and distribution across the world are significant. In European and American Caucasian populations, the 35delG is the most common mutation found to account for nearly 70% of the pathological alleles. Mutations in the GJB6 gene (codifying for Connexin 30) can co-occur in some cases (we refer to the 342-kb truncating deletion, named as GJB6-D13S1830). Thus, these mutations have been associated with autosomal recessive and non-syndromic hearing loss, mostly as biallelic/digenic inheritance of the Cx26 and/or Cx30. Our objective in this study was to describe audiological features and genotypes in patients with GJB2 and/or GJB6 mutations. We performed a retrospective study on a deaf cohort of 566 patients who underwent specific genetic tests for Connexin 26 and 30; the latter was investigated in 385 cases. GJB2 mutations were found in 162 patients and GJB6 mutations in five. The most common mutation of GJB2 was 35delG, a truncating (T) mutation, although we also found other types of truncating (nine genotypes) and non-truncating (NT) (11 genotypes) mutations, such as M34T, L90P, R184P, IVS1 + 1G→A, V37I, and E47X. Even if more than 70% of patients with biallelic/digenic mutations exhibit a severe/profound hearing impairment (even between the simple heterozygotes), mild/moderate deafness is also possible. Other interesting clinical data, such as atypical history or phenotype, were considered. In accordance with the literature, all categories of HL were found. The severe-profound HL was predominant especially in T/T, T/NT forms. The 35delG is the most common mutation that we found, especially in profound hearing impairment. Mild-moderate HL was identified overall among NT/NT forms. Our findings confirm the importance of newborn screening, and the evaluation of genetic mutations to define genotype/phenotype correlation and clinical or audiological features useful to early diagnosis and improvement of therapeutic protocols.

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听力学特征与gjb2、gjb6突变:2003 - 2008年遗传和临床数据的回顾性研究

在世界上许多人群中，GJB2基因(编码连接蛋白26)的突变是常染色体隐性非综合征性听力损失的最常见原因，约占50%的病例。到目前为止，已经确定了100多种(显性或隐性)突变(The Connexin Deafness主页，2009)，世界各地的频率和分布差异是显著的。在欧洲和美国的高加索人群中，35delG是最常见的突变，占病理性等位基因的近70%。GJB6基因的突变(编码Connexin 30)在某些情况下可以同时发生(我们指的是342 kb的截断缺失，命名为GJB6- d13s1830)。因此，这些突变与常染色体隐性遗传和非综合征性听力损失有关，主要是Cx26和/或Cx30的双等位基因/基因遗传。本研究的目的是描述GJB2和/或GJB6突变患者的听力学特征和基因型。我们对566名耳聋患者进行了回顾性研究，这些患者接受了Connexin 26和30的特异性基因检测;后者调查了385例。162例患者发现GJB2突变，5例患者发现GJB6突变。GJB2最常见的突变是35delG，这是一个截断(T)突变，尽管我们也发现了其他类型的截断(9个基因型)和非截断(NT)(11个基因型)突变，如M34T、L90P、R184P、IVS1 + 1G→a、V37I和E47X。即使超过70%的双等位基因/基因突变患者表现出严重/深度听力障碍(即使在简单杂合子之间)，轻度/中度耳聋也是可能的。其他有趣的临床数据，如非典型病史或表型，被考虑。根据文献，我们发现了所有类型的HL。重度重度HL以T/T、T/NT型为主。35delG是我们发现的最常见的突变，尤其是在重度听力障碍中。轻度至中度HL在NT/NT类型中被确定。我们的研究结果证实了新生儿筛查的重要性，以及评估基因突变以确定基因型/表型相关性和临床或听力学特征对早期诊断和改进治疗方案的重要性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Audiological medicine

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