Feng M L, Huang S S, Tang F Z, Zhang X, Li X H, Qiu S W, Yuan Y Y
College of Otolaryngology Head and Neck Surgery, Chinese PLA General Hospital, Chinese PLA Medical School / National Clinical Research Center for Otolaryngologic Diseases / State Key Lab of Hearing Science, Ministry of Education / Beijing Key Lab of Hearing Impairment Prevention and Treatment, Beijing 100853, China.
Department of Otolaryngology-Head and Neck Surgery, the People's Hospital of Guangxi Zhuang Autonomous Region, Nanning 530021, China.
Zhonghua Yi Xue Za Zhi. 2021 Jan 12;101(2):115-121. doi: 10.3760/cma.j.cn112137-20200912-02628.
To perform the phenotype and genetic analysis on two families with moderate sensorineural hearing impairment and determine the cause of deafness. The phenotype and genetic analysis was performed on the two hearing impairment pedigrees coming to Chinese PLA General Hospital from January 2014 to August 2020. DNA samples of the proband from family 1 and the parents from family 2 were collected and tested through next generation sequencing on all deafness genes, and Sanger sequencing was performed to verify the mutation sites. The reported pathogenic variants of the otogelin-like (OTOGL) gene, the autosomal recessive inherited deafness genes that cause moderate sensorineural hearing loss and the clinical manifestations of the deafness genes that have the similar expression location as the OTOGL gene were summarized and analyzed. The pathogenic variants in the families were compound heterozygous variants in the OTOGL gene c.2773C>T/c.2826C>G (p.Arg925*/p.Tyr942*) and c.4455G>A/c.875C>G (Trp1485*/p.Ser292*), respectively. c.2773C>T was an already reported pathogenic variant causing hearing impairment in the literature, while c.2826C>G, c.4455G>A and c.875C>G were novel reported variant sites. The above four variants were classified as pathogenic variants according to the variant interpretation standards and guideline of the Amercian College of Medical Genetics and Genomics. Pathogenic variants in OTOGL gene is an important genetic factor leading to moderate sensorineural hearing loss. The newly discovered variant sites c.2826C>G, c.4455G>A and c.875C>G enrich the variant spectrum of OTOGL gene. The results of the current study provide a basis for genetic counseling of the related families and a new target for the treatment of hereditary hearing loss in the future.
对两个中度感音神经性听力损失家庭进行表型和基因分析,以确定耳聋原因。对2014年1月至2020年8月来中国人民解放军总医院就诊的两个听力损失家系进行表型和基因分析。收集了家系1先证者和家系2父母的DNA样本,通过对所有耳聋基因进行二代测序进行检测,并采用桑格测序法验证突变位点。总结并分析了耳胶样蛋白(OTOGL)基因(导致中度感音神经性听力损失的常染色体隐性遗传性耳聋基因)的已报道致病变异以及与OTOGL基因表达位置相似的耳聋基因的临床表现。家系中的致病变异分别为OTOGL基因c.2773C>T/c.2826C>G(p.Arg925*/p.Tyr942*)和c.4455G>A/c.875C>G(Trp1485*/p.Ser292*)的复合杂合变异。c.2773C>T是文献中已报道的导致听力损失的致病变异,而c.2826C>G、c.4455G>A和c.875C>G是新报道的变异位点。根据美国医学遗传学与基因组学学会的变异解读标准和指南,上述四个变异被分类为致病变异。OTOGL基因中的致病变异是导致中度感音神经性听力损失的重要遗传因素。新发现的变异位点c.2826C>G、c.4455G>A和c.875C>G丰富了OTOGL基因的变异谱。本研究结果为相关家系的遗传咨询提供了依据,并为未来遗传性听力损失的治疗提供了新靶点。
