Whole-exome sequencing of de novo genetic variants in a Chinese family with a sporadic case of congenital nonsyndromic hearing loss

Sijing Hu; Hao Zhang; Yunqiang Liu; Mohan Liu; Jingjing Li; Shunyao Liao

doi:10.12688/f1000research.27739.2

Whole-exome sequencing of de novo genetic variants in a Chinese family with a sporadic case of congenital nonsyndromic hearing loss

F1000Res. 2021 Feb 2:10:61. doi: 10.12688/f1000research.27739.2. eCollection 2021.

Authors

Sijing Hu¹, Hao Zhang², Yunqiang Liu², Mohan Liu², Jingjing Li¹, Shunyao Liao¹

Affiliations

¹ Diabetes Center & Institute of Organ Transplantation, Sichuan Provincial People's Hospital, University of Electronic Science and Technology of China, Chengdu, China, 610072, China.
² Department of Medical Genetics and Division of Morbid Genomics, State Key Laboratory of Biotherapy, West China Hospital,, West China Medical School, Sichuan University,, Chengdu, China, 610041, China.

Abstract

Background: We examined the genetic variants of a Chinese family with a 22-month-old infant with sporadic non-syndromic sensorineural hearing loss (NSHL). Methods: The whole-exome sequence data in the family, especially the de novo variants presented in the patient, were analyzed and the effect of the disease-causing genetic variants on the protein expression level and cellular localization were examined by cell-based functional assay. Results: The infant had no known NSHL-causing variants, except two compound heterozygous variants in connexin26 gene GJB2; one was the c.79G>A, c.341A>G haplotype from the asymptomatic mother who was benign, and the other was a de novo pathogenic c.262G>C (p.A88P). In vitro, GJB2 with c.262G>C was weakly expressed and displayed a punctate distribution in the cytoplasm and cytomembrane, while wild type GJB2 was robustly expressed in the cytomembrane. We deduced that the de novo pathogenic GJB2 c.262G>C exacerbated loss-of-function in the context of leaky variants c.79G>A, c.341A>G in the patient. Interestingly, further analysis of exome sequences revealed that the occurrence of de novo pathogenic variants in the infant was frequent. Among the total~47,000 variants, 143 were de novo in the patient, whereas among all 74 variants predicted to be pathogenic/likely pathogenic, 21 were heterozygous and two were homozygous de novo. The occurrence rate of de novo deleterious variants was much higher (31.1%, 23/74) than that in total (0.34%, 143/47,000). It is notable that most genes with de novo deleterious variants were environment-sensitive, such as GJB2, MNK1, MNK2, MUC4, RAD21 and DNA copy number variations. Conclusions: The full picture of genetic variants in the exome might help us to interpret the NSHL-causing variants. More research is needed into the causes of de novo deleterious variants and gene-environment interactions in congenital NSHL.

Keywords: Whole-exome sequencing; compound heterozygosity; de novo pathogenic variant; genetic and environmental interaction; nonsyndromic hearing loss.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

China
DNA Copy Number Variations*
Deafness
Exome Sequencing
Hearing Loss, Sensorineural* / genetics
Humans
Infant
Mutation
Pedigree

Supplementary concepts

Nonsyndromic Deafness

Grants and funding

This work was supported by grants from the National Natural Science Foundation of China (grant numbers: 81471430 and 81773159). The funding sponsors had no involvement in the research design, data processing, report writing or publication.