Updates on Genetic Hearing Loss: From Diagnosis to Targeted Therapies

Author:

Yun YejinORCID,Lee Sang-YeonORCID

Abstract

Sensorineural hearing loss (SNHL) is the most common sensory disorder, with a high Mendelian genetic contribution. Considering the genotypic and phenotypic heterogeneity of SNHL, the advent of next-generation sequencing technologies has revolutionized knowledge on its genomic architecture. Nonetheless, the conventional application of panel and exome sequencing in real-world practice is being challenged by the emerging need to explore the diagnostic capability of whole-genome sequencing, which enables the detection of both noncoding and structural variations. Small molecules and gene therapies represent good examples of how breakthroughs in genetic understanding can be translated into targeted therapies for SNHL. For example, targeted small molecules have been used to ameliorate autoinflammatory hearing loss caused by gain-of-function variants of <i>NLRP3</i> and inner ear proteinopathy with <i>OSBPL2</i> variants underlying dysfunctional autophagy. Strikingly, the successful outcomes of the first-in-human trial of <i>OTOF</i> gene therapy highlighted its potential in the treatment of various forms of genetic hearing loss. clustered regularly interspaced short palindromic repeats (CRISPR)-based technologies are currently being developed for site-specific genome editing to treat human genetic disorders. These advancements have led to an era of genotype- and mechanism-based precision medicine in SNHL practice.

Funder

Seoul National University Hospital

National Research Foundation of Korea

Ministry of Education

Publisher

The Korean Audiological Society

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