Jin Young Ju, Park Jaehong, Kim Ah Reum, Rah Yoon Chan, Choi Byung Yoon
Department of Otorhinolaryngology-Head and Neck Surgery, Seoul National University Hospital, Seoul National University College of Medicine, Seoul, Republic of Korea.
Department of Otorhinolaryngology-Head and Neck Surgery, Seoul National University Bundang Hospital, Seoul National University College of Medicine, Seongnam, Republic of Korea.
Int J Pediatr Otorhinolaryngol. 2014 Jul;78(7):1030-5. doi: 10.1016/j.ijporl.2014.03.033. Epub 2014 Apr 24.
(1) To describe the frequency of the OTOF mutations among Korean ARNSHL (autosomal recessive nonsyndromic hearing loss) populations; (2) to report the vertical transmission of DFNB9 in a family, where two related DFNB9 patients in the family manifested a different audiological phenotype.
We analyzed the prevalence of OTOF mutations among 71 Korean sporadic or possible ARNSHL pediatric patients, as well as among AN/AD (auditory neuropathy/auditory dys-synchrony) patients by direct PCR (polymerase chain reaction) sequencing or targeted resequencing of known deafness genes.
The AN/AD phenotype which was characterized by preservation of OAE (otoacoustic emission) was present in 5 (7%) of 71 probands, and the prevalence of OTOF mutations was calculated to be 20% (1/5) and 1.4% (1/71) among AN/AD patients and total sporadic/ARNSHL patients, respectively. PJVK mutations did not account for Non-DFNB9 AN/AD patients. To our interest, the only proband (SB4-11) with two OTOF mutant alleles in our cohort had deaf parents, who also turned out to be DFNB9. We identified a novel splice site variant of OTOF from the mother (SB4-13) of SB4-11. This was the first observation of vertical transmission of DFNB9 phenotype from parents to son in this population where the prevalence of OTOF is very low and consanguineous marriage is not allowed. Another DFNB9 patient (SB4-12), the father of SB4-11, carried a homozygous p.Y374X mutation that affected only the long isoform of OTOF and did not manifest AN/AD.
The OTOF mutations do not contribute significantly to Korean ARNSHL and AN/AD unlike in Japan and Taiwan. This low prevalence mandates a search for other etiologies. Our observation of the discordant audiologic phenotype within the same DFNB9 family is more likely due to the loss of OAE over time rather than a genotype-phenotype correlation.
(1)描述韩国常染色体隐性非综合征性听力损失(ARNSHL)人群中OTOF突变的频率;(2)报告一个家族中DFNB9的垂直遗传情况,该家族中有两名相关的DFNB9患者表现出不同的听力学表型。
我们通过直接PCR(聚合酶链反应)测序或对已知耳聋基因进行靶向重测序,分析了71例韩国散发性或可能为ARNSHL的儿科患者以及听觉神经病/听觉失同步(AN/AD)患者中OTOF突变的患病率。
71名先证者中有5名(7%)表现出以耳声发射(OAE)保留为特征的AN/AD表型,在AN/AD患者和总的散发性/ARNSHL患者中,OTOF突变的患病率分别计算为20%(1/5)和1.4%(1/71)。PJVK突变不能解释非DFNB9的AN/AD患者。有趣的是,在我们的队列中,唯一携带两个OTOF突变等位基因的先证者(SB4-11)的父母是耳聋患者,结果也证实他们是DFNB9。我们从SB4-11的母亲(SB4-13)中鉴定出一种新的OTOF剪接位点变异。这是在OTOF患病率极低且不允许近亲结婚的人群中首次观察到DFNB9表型从父母垂直遗传给儿子。另一名DFNB9患者(SB4-12)是SB4-11的父亲,携带纯合的p.Y374X突变,该突变仅影响OTOF的长异构体,且未表现出AN/AD。
与日本和台湾不同,OTOF突变对韩国的ARNSHL和AN/AD贡献不大。这种低患病率促使人们寻找其他病因。我们在同一个DFNB9家族中观察到的不一致听力学表型更可能是由于OAE随时间丧失,而非基因型-表型相关性。
