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The Many Faces of DFNB9: Relating

机译:DFNB9的许多面孔:相关

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摘要

The OTOF gene encodes otoferlin, a critical protein at the synapse of auditory sensory cells, the inner hair cells (IHCs). In the absence of otoferlin, signal transmission of IHCs fails due to impaired release of synaptic vesicles at the IHC synapse. Biallelic pathogenic and likely pathogenic variants in OTOF predominantly cause autosomal recessive profound prelingual deafness, DFNB9. Due to the isolated defect of synaptic transmission and initially preserved otoacoustic emissions (OAEs), the clinical characteristics have been termed “auditory synaptopathy”. We review the broad phenotypic spectrum reported in patients with variants in OTOF that includes milder hearing loss, as well as progressive and temperature-sensitive hearing loss. We highlight several challenges that must be addressed for rapid clinical and genetic diagnosis. Importantly, we call for changes in newborn hearing screening protocols, since OAE tests fail to diagnose deafness in this case. Continued research appears to be needed to complete otoferlin isoform expression characterization to enhance genetic diagnostics. This timely review is meant to sensitize the field to clinical characteristics of DFNB9 and current limitations in preparation for clinical trials for OTOF gene therapies that are projected to start in 2021.
机译:OFOF基因编码Otoferlin,在听觉感觉细胞突触的关键蛋白质,内毛细胞(IHC)。在没有otoferlin的情况下,由于IHC Synapse在IHC Synapse的突触囊泡的释放受损,IHCs的信号传输失败。奥氏炎的双层致病和可能的致病变体主要导致常染色体隐性深刻的前期耳聋,DFNB9。由于突触传递的分离缺陷和最初保存的耳声发射(OAES),临床特征已被称为“听觉突触疗法”。我们审查了在OTOF中变种患者报告的广泛表型谱,包括MILDER听力损失,以及渐进和温度敏感的听力损失。我们强调了必须解决的若干挑战,以便快速临床和遗传诊断。重要的是,我们要求新生儿听证筛查方案的变化,因为OAE测试在这种情况下未能诊断耳聋。仍然需要进行持续的研究来完成OTOFERLIN同种型表达表征以增强遗传诊断。该及时审查意味着将现场敏感于DFNB9的临床特征和当前限制,以准备临床试验,用于在2021年开始的OTOF基因疗法的临床试验。

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