Behlouli Asma, Bonnet Crystel, Abdi Samia, Bouaita Aïcha, Lelli Andrea, Hardelin Jean-Pierre, Schietroma Cataldo, Rous Yahia, Louha Malek, Cheknane Ahmed, Lebdi Hayet, Boudjelida Kamel, Makrelouf Mohamed, Zenati Akila, Petit Christine
INSERM UMRS1120, UPMC, Institut de la Vision, Paris, France.
Orphanet J Rare Dis. 2014 Apr 17;9:55. doi: 10.1186/1750-1172-9-55.
Almost 90% of all cases of congenital, non-syndromic, severe to profound inherited deafness display an autosomal recessive mode of transmission (DFNB forms). To date, 47 causal DFNB genes have been identified, but many others remain to be discovered. We report the study of two siblings born to consanguineous Algerian parents and affected by isolated, profound congenital deafness.
Whole-exome sequencing was carried out on these patients after a failure to identify mutations in the DFNB genes frequently involved.
A biallelic nonsense mutation, c.88C > T (p.Gln30*), was identified in EPS8 that encodes epidermal growth factor receptor pathway substrate 8, a 822 amino-acid protein involved in actin dynamics. This mutation predicts a truncated inactive protein or no protein at all. The mutation was also present, in the heterozygous state, in one clinically unaffected sibling and in both unaffected parents, and was absent from the other two unaffected siblings. It was not found in 120 Algerian normal hearing control individuals or in the Exome Variant Server database. EPS8 is an F-actin capping and bundling protein. Mutant mice lacking EPS8 (Eps8-/- mice), which is present in the hair bundle, the sensory antenna of the auditory sensory cells that operate the mechano-electrical transduction, are also profoundly deaf and have abnormally short hair bundle stereocilia.
This new DFNB form is likely to arise from abnormal hair bundles resulting in compromised detection of physiological sound pressures.
几乎所有先天性、非综合征性、重度至极重度遗传性耳聋病例的90%呈现常染色体隐性遗传模式(DFNB型)。迄今为止,已鉴定出47个致病DFNB基因,但仍有许多其他基因有待发现。我们报告了对一对出生于近亲结婚的阿尔及利亚父母的兄弟姐妹的研究,他们患有孤立性重度先天性耳聋。
在未能在常见的DFNB基因中鉴定出突变后,对这些患者进行了全外显子组测序。
在编码表皮生长因子受体通路底物8(一种参与肌动蛋白动力学的含822个氨基酸的蛋白质)的EPS8中鉴定出双等位基因无义突变c.88C>T(p.Gln30*)。该突变预测会产生截短的无活性蛋白或根本不产生蛋白。该突变也以杂合状态存在于一名临床未受影响的兄弟姐妹以及两名未受影响的父母中,而在另外两名未受影响的兄弟姐妹中不存在。在120名阿尔及利亚听力正常的对照个体或外显子变体服务器数据库中未发现该突变。EPS8是一种F-肌动蛋白封端和捆绑蛋白。缺乏EPS8的突变小鼠(Eps8-/-小鼠),EPS8存在于毛束中,毛束是听觉感觉细胞的感觉触角,负责机械-电转换,这些小鼠也严重耳聋且毛束静纤毛异常短。
这种新的DFNB型可能源于异常的毛束,导致对生理声压的检测受损。
