Your search keyword '"Bai, Xiaohui"' showing total 8 results

1. A novel MYH14 mutation in a Chinese family with autosomal dominant nonsyndromic hearing loss.

Author

Wang, Mingming, Zhou, Yicui, Zhang, Fengguo, Fan, Zhaomin, Bai, Xiaohui, and Wang, Haibo

Subjects

HEARING disorders, RECESSIVE genes, GENETIC mutation, NOISE-induced deafness, MISSENSE mutation, GENETIC disorders

Abstract

Background: MYH14 gene mutations have been suggested to be associated with nonsyndromic/syndromic sensorineural hearing loss. It has been reported that mutations in MYH14 can result in autosomal dominant nonsyndromic deafness-4A (DFNA4). Methods: In this study, we examined a four-generation Han Chinese family with nonsyndromic hearing loss. Targeted next-generation sequencing of deafness genes was employed to identify the pathogenic variant. Sanger sequencing and PCR-RFLP analysis were performed in affected members of this family and 200 normal controls to further confirm the mutation. Results: Four members of this family were diagnosed as nonsyndromic bilateral sensorineural hearing loss with postlingual onset and progressive impairment. A novel missense variant, c.5417C > A (p.A1806D), in MYH14 in the tail domain of NMH II C was successfully identified as the pathogenic cause in three affected individuals. The family member II-5 was suggested to have noise-induced deafness. Conclusion: In this study, a novel missense mutation, c.5417C > A (p.A1806D), in MYH14 that led to postlingual nonsyndromic autosomal dominant SNHL were identified. The findings broadened the phenotype spectrum of MYH14 and highlighted the combined application of gene capture and Sanger sequencing is an efficient approach to screen pathogenic variants associated with genetic diseases. [ABSTRACT FROM AUTHOR]

Published

2020

2. Identification of two novel mutations in POU4F3 gene associated with autosomal dominant hearing loss in Chinese families.

Author

Bai, Xiaohui, Zhang, Fengguo, Xiao, Yun, Jin, Yu, Zheng, Qingyin, Wang, Haibo, and Xu, Lei

Subjects

RECESSIVE genes, HEARING disorders, GENETIC mutation, FRAMESHIFT mutation, PROTEIN structure, MOLECULAR weights

Abstract

Autosomal dominant non‐syndromic hearing loss is genetically heterogeneous with 47 genes identified to date, including POU4F3. In this study, by using a next‐generation sequencing panel targeting 127 deafness genes, we identified a pathogenic frameshift mutation c.704_705del and a missense mutation c.593G>A in two three‐generation Chinese families with late‐onset progressive ADNSHL, respectively. The novel mutations of POU4F3 co‐segregated with the deafness phenotype in these two families. c.704_705del caused a frameshift p.T235fs and c.593G>A caused an amino acid substitution of p.R198H. Both mutations led to an abnormal and incomplete protein structure. POU4F3 with either of the two mutations was transiently transfected into HEI‐OC1 and HEK 293 cell lines and immunofluorescence assay was performed to investigate the subcellular localization of mutated protein. The results indicated that both c.704_705del (p.T235fs) and c.593G>A (p.R198H) could impair the nuclear localization function of POU4F3. The p.R198H POU4F3 protein was detected as a weak band of the correct molecular weight, indicating that the stability of p.R198H POU4F3 differed from that of the wild‐type protein. While, the p.T235fs POU4F3 protein was expressed with a smaller molecular weight, implying this mutation result in a frameshift and premature termination of the POU4F3 protein. In summary, we report two novel mutations of POU4F3 associated with progressive ADNSHL and explored their effects on POU4F3 nuclear localization. These findings expanded the mutation spectrum of POU4F3 and provided new knowledge for the pathogenesis of POU4F3 in hearing loss. [ABSTRACT FROM AUTHOR]

Published

2020

3. Mitochondrial tRNA mutations in 887 Chinese subjects with hearing loss.

Author

Zheng, Jing, Bai, Xiaohui, Xiao, Yun, Ji, Yanchun, Meng, Feilong, Aishanjiang, Maerhaba, Gao, Yinglong, Wang, Haibo, Fu, Yong, and Guan, Min-Xin

Subjects

*TRANSFER RNA, *HEARING disorders, *CHINESE people, *NUCLEOTIDES, *PATHOLOGY, *HAIR cells, *FUNCTIONAL analysis

Abstract

• 147 mitochondrial tRNA variants were identified in 887 Chinese Subjects with hearing loss. • 39 tRNA mutations (10 pathogenic and 29 likely pathogenic) were identified as putative deafness-associated tRNA variants. • 4.96% of the individuals carried the pathogenic/likely pathogenic tRNA mutations. • The mitochondrial tRNA mutations are the important causes of hearing loss. Mutations in the mitochondrial tRNAs have been reported to be the important cause of hearing loss. However, only a few cases have been identified thus far and the prevalence of mitochondrial tRNA mutations in hearing-impaired patients remain unclear. Here we performed the mutational analysis of 22 mitochondrial tRNA genes in a large cohort of 887 Han Chinese subjects with hearing loss by Sanger sequencing. The systemic evaluation of putative pathogenic variants was further carried out by frequency in controls (<1%), phylogenetic analysis, structural analysis and functional prediction. As a result, a total of 147 variants on 22 tRNA genes were identified. Among these, 39 tRNA mutations (10 pathogenic and 29 likely pathogenic) which absent or present <1% in 773 Chinese controls, localized at highly conserved nucleotides, or changed the modified nucleotides, could have potential structural alterations and functional significance, thereby considered to be deafness-associated mutations. Furthermore, 44 subjects carried one of these 39 pathogenic/likely pathogenic tRNA mutations with a total prevalence of 4.96%. However, the phenotypic variability and incomplete penetrance of hearing loss in pedigrees carrying these tRNA mutations indicate the involvement of modifier factors, such as nuclear encoded genes associated with mitochondrion biogenesis, mitochondrial haplotypes, epigenetic and environmental factors. Thus, our data provide the evidence that mitochondrial tRNA mutations are the important causes of hearing loss among Chinese population. These findings further increase our knowledge on the clinical relevance of tRNA mutations in the mitochondrial genome, and should be helpful to elucidate the pathogenesis of maternal hearing loss. [ABSTRACT FROM AUTHOR]

Published

2020

4. Five Novel Mutations in LOXHD1 Gene Were Identified to Cause Autosomal Recessive Nonsyndromic Hearing Loss in Four Chinese Families.

Author

Bai, Xiaohui, Zhang, Chi, Zhang, Fengguo, Xiao, Yun, Jin, Yu, Wang, Haibo, and Xu, Lei

Subjects

*GENETICS of deafness, *CARRIER proteins, *HEARING disorders, *GENETIC mutation, *SEVERITY of illness index, *SEQUENCE analysis, *CORNEAL dystrophies, *GENOTYPES

Abstract

Hearing loss is one of the most common sensory disorders in newborns and is mostly caused by genetic factors. Autosomal recessive nonsyndromic hearing loss (ARNSHL) is usually characterized as a severe-to-profound congenital sensorineural hearing loss and later can cause various degrees of defect in the language and intelligent development of newborns. The mutations in LOXHD1 gene have been shown to cause DFNB77, a type of ARNSHL. To date, there are limited reports about the association between LOXHD1 gene and ARNSHL. In this study, we reported six patients from four Chinese families suffering from severe-to-profound nonsyndromic hearing loss. We performed targeted next generation sequencing in the six affected members and identified five novel pathogenic mutations in LOXHD1 including c.277G>A (p.D93N), c.611-2A>T, c.1255+3A>G, c.2329C>T (p.Q777 ∗ ), and c.5888delG (p.G1963Afs ∗ 136). These mutations were confirmed to be cosegregated with the hearing impairment in the families by Sanger sequencing and were inherited in an autosomal recessive pattern. All of the five mutations were absent in 200 control subjects. There were no symptoms of Fuchs corneal dystrophy in the probands and their blood-related relatives. We concluded that these five novel mutations could be involved in the underlying mechanism resulting in the hearing loss, and this discovery expands the genotypic spectrum of LOXHD1 mutations. [ABSTRACT FROM AUTHOR]

Published

2020

5. Three MYO15A Mutations Identified in One Chinese Family with Autosomal Recessive Nonsyndromic Hearing Loss.

Author

Zhang, Fengguo, Xu, Lei, Xiao, Yun, Li, Jianfeng, Bai, Xiaohui, and Wang, Haibo

Subjects

HEARING disorders, SENSORY disorders, PHYLOGENETIC models, GENETIC mutation, DIAGNOSIS, THERAPEUTICS

Abstract

Hearing impairment is one of the most common sensory disease, of which more than 50% is attributed to a genetic etiology. The goal of this research is to explore the genetic cause of a Chinese deafness pedigree who was excluded of GJB2, SLC26A4, or MtDNA12SrRNA variants. Three variants, c.3971C>A (p.A1324D), c.4011insA (p.Q1337Qfs∗22), and c.9690+1G>A, in the MYO15A gene were identified by targeted capture sequencing and Sanger sequencing, and the first two of them were novel. These variants were cosegregated with the disease in this family and absent in 200 normal hearing persons. They were concluded to be pathogenic mutations by phylogenetic analysis and structure modeling. Thus, the combined use of SNPScan assay and targeted capture sequencing is a high-efficiency and cost-effective screening procedure for hereditary hearing loss. Genetic counseling would be important for this family, and our finding would be a great supplement to the mutation spectrum of MYO15A. [ABSTRACT FROM AUTHOR]

Published

2018

6. GJB2, SLC26A4 , and mitochondrial DNA12S rRNA hot-spots in 156 subjects with non-syndromic hearing loss in Tengzhou, China.

Author

Ma, Yalin, Xiao, Yun, Bai, Xiaohui, Zhang, Fengguo, Zhang, Daogong, Xu, Xinmao, Xu, Lei, and Wang, Haibo

Subjects

HEARING disorders, DNA analysis, CHI-squared test, GENES, GENETIC polymorphisms, LONGITUDINAL method, GENETIC mutation, PROBABILITY theory, RESEARCH funding, GENETIC testing, DATA analysis software, GENOTYPES, GENETICS

Abstract

Conclusion: In this cohort of 156 non-syndromic hearing-impaired subjects of Tengzhou area, the most common deafness-associated genesGJB2,SLC26A4andmtDNA 12S rRNAwere investigated by SNPscan efficiently.GJB2c.235delC andSLC26A4c.IVS7-2A > G were the most common mutation sites.Objectives: Until now, there is no systematic gentic analysis in patients with non-syndromic hearing loss for Tengzhou area, so we evaluated the molecular etiology to investigate the hot-sports.Methods: Peripheral blood samples were obtained from 156 patients with severe-to-profound non-syndromic deafness in Tengzhou. The SNP scan assay technique was performed for a rapid multiplex genetic screening to detect the 115 mutations of the most common three genes. All results were statistically analyzed with SPSS software.Results: Among the 156 analyzed patients, 60 patients were demonstrated with deafness genes, accounting for 38.46% (60/156), includingGJB2(22.44%, 35/156),SLC26A4(13.66%, 22/156), andmtDNA 12S rRNA(2.56%, 4/156). In this study, we confirmed 23 deafness-causing mutations and 27 different allelic combinations includingGJB2(eight variants, 11 allelic combinations),SLC26A4(13 variants, 16 allelic combinations) andmtDNA 12S rRNA(two variants). The occurrence rates of these deafness-causing mutationsGJB2c.235delC andSLC26A4c.IVS7-2A > G were significantly higher than other mutation sites (p < 0.01). [ABSTRACT FROM PUBLISHER]

Published

2016

7. Mutation Analysis of the Common Deafness Genes in Patients with Nonsyndromic Hearing Loss in Linyi by SNPscan Assay.

Author

Zhang, Fengguo, Xiao, Yun, Xu, Lei, Zhang, Xue, Zhang, Guodong, Li, Jianfeng, Lv, Huaiqing, Bai, Xiaohui, and Wang, Haibo

Subjects

GENETICS of deafness, DNA analysis, ALLELES, BIOLOGICAL assay, CHILDREN'S hospitals, HEARING disorders, MEDICAL cooperation, GENETIC mutation, POLYMERASE chain reaction, QUESTIONNAIRES, RESEARCH, RESEARCH funding, SPECIAL education schools, DISEASE prevalence, DATA analysis software, DESCRIPTIVE statistics

Abstract

Hearing loss is a common sensory disorder, and at least 50% of cases are due to a genetic etiology. Although hundreds of genes have been reported to be associated with nonsyndromic hearing loss, GJB2, SLC26A4, and mtDNA12SrRNA are the major contributors. However, the mutation spectrum of these common deafness genes varies among different ethnic groups. The present work summarized mutations in these three genes and their prevalence in 339 patients with nonsyndromic hearing loss at three different special education schools and one children’s hospital in Linyi, China. A new multiplex genetic screening system “SNPscan assay” was employed to detect a total of 115 mutations of the above three genes. Finally, 48.67% of the patients were identified with hereditary hearing loss caused by mutations in GJB2, SLC26A4, and mtDNA12SrRNA. The carrying rate of mutations in the three genes was 37.76%, 19.75%, and 4.72%, respectively. This mutation profile in our study is distinct from other parts of China, with high mutation rate of GJB2 suggesting a unique mutation spectrum in this area. [ABSTRACT FROM AUTHOR]

Published

2016

8. Erratum to “A Novel Nonsense Mutation of POU4F3 Gene Causes Autosomal Dominant Hearing Loss”.

Author

Zhang, Chi, Wang, Mingming, Xiao, Yun, Zhang, Fengguo, Zhou, Yicui, Li, Jianfeng, Zheng, Qingyin, Bai, Xiaohui, and Wang, Haibo

Subjects

HEARING disorders, GENETIC mutation, PROGNOSIS, PHYSIOLOGY

Published

2017