Non-syndromic autosomal dominant progressive non-specific mid-frequency sensorineural hearing impairment with childhood to late adolescence onset (DFNA21).

H Kunst, H Marres, P Huygen, G van Duijnhoven, A Krebsova, S van der Velde, A Reis, F Cremers, C Cremers
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引用次数: 39

Abstract

An autosomal dominant trait of progressive, non-syndromic, non-specific mid-frequency sensorineural hearing impairment was identified in a Dutch family. Many affected family members (n = 21) were identified, among whom seven out of nine relatives aged < 30 years do not show pure mid-frequency hearing impairment, which suggests variable expression. Regression analysis was used to evaluate the age-related hearing threshold data in a cross-sectional analysis in 24 affected patients and in a longitudinal analysis in five of these. At all frequencies, progression in hearing impairment (i.e. the regression coefficient) was significant and fairly similar: the pooled value was about 1.0 dB/y. There was no significant (i.e. not =0 dB) offset threshold (i.e. Y intercept at age 0) found at any frequency. The regression lines could be pooled for the low frequencies (0.25-0.5 kHz) and the mid/high frequencies (1-8 kHz) and this produced apparent onset ages of about 3 and 4 years and annual threshold increases of 0.75 and 1.1 dB/y, respectively. In most patients there is a relatively late onset age (maximum in the range of at least 25-45 years). However, based on the longitudinal analysis of a patient from the age of 4 years onwards in some patients sensorineural hearing impairment might be congenital/prelingual. Oculo-vestibular function was found to be normal. Results from linkage studies tentatively position the underlying gene defect telomeric to the repositioned DFNA13 locus at chromosome 6p21-22.

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儿童期至青春期晚期发病的非综合征性常染色体显性进行性非特异性中频感音神经性听力障碍(DFNA21)。
在一个荷兰家庭中发现了进行性,非综合征性,非特异性中频感音神经性听力障碍的常染色体显性特征。许多受影响的家庭成员(n = 21)被确定,其中9名年龄< 30岁的亲属中有7名没有表现出纯粹的中频听力障碍,这表明表达是可变的。在24例患者的横断面分析和其中5例患者的纵向分析中,使用回归分析来评估与年龄相关的听力阈值数据。在所有频率下,听力损伤的进展(即回归系数)显著且相当相似:汇总值约为1.0 dB/y。在任何频率上都没有发现显著的(即不=0 dB)偏移阈值(即0岁时的Y截距)。低频率(0.25 ~ 0.5 kHz)和中高频率(1 ~ 8 kHz)的回归线可以合并,这产生了大约3年和4年的明显发病年龄,年阈值分别增加0.75和1.1 dB/y。在大多数患者中,发病年龄相对较晚(最多在25-45岁之间)。然而,根据对4岁以上患者的纵向分析,一些患者的感音神经性听力障碍可能是先天性的/语前性的。眼前庭功能正常。连锁研究的结果初步将潜在的基因缺陷端粒定位在染色体6p21-22上重新定位的DFNA13位点。
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