Your search keyword '"Su, Jiasun"' showing total 10 results

1. Two novel compound heterozygous variants of LTBP4 in a Chinese infant with cutis laxa type IC and a review of the related literature.

Author

Zhang, Qiang, Qin, Zailong, Yi, Shang, Wei, Hao, Zhou, Xun Zhao, and Su, Jiasun

Subjects

SKIN, INFANTS, GENETIC mutation, LITERATURE reviews, DATABASE management software, FACIOSCAPULOHUMERAL muscular dystrophy

Abstract

Background: Autosomal recessive cutis laxa type IC (ARCL IC, MIM: #613177) results from a mutation in the LTBP4 gene (MIM: #604710) on chromosome 19q13. Case presentation: A 28-day-old Chinese infant with generalized cutis laxa accompanied by impaired pulmonary, gastrointestinal, genitourinary, retinal hemorrhage, abnormality of coagulation and hyperbilirubinemia was admitted to our hospital. To find out the possible causes of these symptoms, whole-exome sequencing was performed on the infant. Two novel pathogenic frame-shift variants [c.605_606delGT (p.Ser204fs * 8) and c.1719delC (p.Arg574fs * 199)] of the LTBP4 gene associated with ARCL IC were found which was later verified by Sanger sequencing. The pathogenicity of mutations was subsequently assessed by several software programs and databases. In addition, an analytical review on the clinical phenotypes of the disease previously reported in literature was performed. Conclusions: This is the first report of a Chinese infant with ARCL IC in China due to novel pathogenic variations of LTBP4. Our study extends the cutis laxa type IC mutation spectrum as well as the phenotypes associated with the disease in different populations. [ABSTRACT FROM AUTHOR]

Published

2020

2. Clinical application of whole-exome sequencing: A retrospective, single-center study.

Author

Zhang, Qiang, Qin, Zailong, Yi, Shang, Wei, Hao, Zhou, Xun Zhao, and Su, Jiasun

Subjects

MEDICAL personnel, PHENOTYPES, MISSENSE mutation, GENETIC mutation, GENETIC disorders, AUDITORY neuropathy

Abstract

The aim of the present study was to assess the practical diagnostic value of whole-exome sequencing (WES) in patients with different phenotypes and to explore possible strategies to increase the capability of WES in identifying disease-causing genes. A total of 1,360 patients (aged from 1 day to 42 years old) with manifestations of genetic diseases were genotyped using WES and statistical analysis was performed on the results obtained. Within this cohort, the overall positive rate of identification of a disease-causing gene alteration was 44.41%. The positive identification rate where trio-samples were used (from the proband and both parents) was higher than that where a single proband sample was used (50.00 vs. 43.71%), and 604 positive cases with 150 genetic syndromes, 510 genes and 718 mutations were detected. Missense mutations were the most common variations (n=335, 45.27%) and visual or auditory abnormalities (58.51%) had the highest rate of association with a genetic abnormality. The positive detection rate of WES was elevated with the increase in the number of clinical symptoms from 1 to 8. The present study indicated that WES may be used as a valuable tool in the clinic and the positive rate depends more on the professional experience of clinicians rather than on the analytical capabilities of the data analyst. At the same time, particular attention must be paid to certain possible factors (such as the age of the patients as well as possible exon deletions), which may affect the diagnostic rate while applying this process. [ABSTRACT FROM AUTHOR]

Published

2021

3. Novel pathogenic ACAN variants in non-syndromic short stature patients.

Author

Hu, Xuyun, Gui, Baoheng, Su, Jiasun, Li, Hongdou, Li, Niu, Yu, Tingting, Zhang, Qinle, Xu, Yufei, Li, Guoqiang, Chen, Yulin, Qing, Yanrong, Li, Chuan, Luo, Jingsi, Fan, Xin, Ding, Yu, Li, Juan, Wang, Jian, Wang, Xiumin, Chen, Shaoke, and Shen, Yiping

Subjects

*SHORT stature, *GENETIC mutation, *SKELETAL maturity, *PHENOTYPES, *DISEASE prevalence, *GENETICS

Abstract

Background Pathogenic variants of ACAN have been reported to cause spondyloepiphyseal dysplasia Kimberley type, spondyloepimetaphyseal dysplasia, familial osteochondritis dissecans and idiopathic short stature with normal to advanced bone age. A recent international cohort study significantly expanded the ACAN mutation spectrum, further delineated the heterogeneous clinical characteristics of ACAN mutation patients. The prevalence of ACAN mutation in short stature patients is yet unknown. Methods Here we set to assess the frequency of ACAN variants among a cohort of 218 Chinese children with non-syndromic short stature. Results We identified three novel truncating variants at the 5′ end of ACAN gene. All these pathogenic variants co-segregate with severe short stature phenotype in families. In addition, none of the probands showed significant advanced bone age. All affected individuals showed no signs of significant dysmorphic features or skeletal abnormities. The prevalence of ACAN defect in this cohort is estimated to be 1.4% (3/218). It is higher among families with parents also affected with severe short stature, up to 7.0% (3/43) if parental height is < 2.5 SD or 16.7% (3/18) if parental height is < 3.0 SD. Conclusion Our data suggest that ACAN mutation is a relative common cause of familial severe short stature. [ABSTRACT FROM AUTHOR]

Published

2017

4. Targeted addition of mini-dystrophin into rDNA locus of Duchenne muscular dystrophy patient-derived iPSCs.

Author

Zeng, Baitao, Zhou, Miaojin, Liu, Bo, Shen, Fei, Xiao, Rou, Su, Jiasun, Hu, Zhiqing, Zhang, Yiti, Gu, Ao, Wu, Lingqian, Liu, Xionghao, and Liang, Desheng

Subjects

*DUCHENNE muscular dystrophy, *INDUCED pluripotent stem cells, *DYSTROPHIN genes, *RECOMBINANT DNA, *LOCUS (Genetics), *GENETIC mutation, *RIBOSOMAL DNA

Abstract

Duchenne muscular dystrophy (DMD), the most common lethal muscular disorder, affects 1 in 5000 male births. It is caused by mutations in the X-linked dystrophin gene (DMD), and there is no effective treatment currently. Gene addition is a promising strategy owing to its universality for patients with all gene mutations types. In this study, we describe a site-specific gene addition strategy in induced pluripotent stem cells (iPSCs) derived from a DMD patient with exon 50 deletion. By using transcription activator-like effector nickases (TALENickases), the mini-dystrophin cassette was precisely targeted at the ribosomal RNA gene (rDNA) locus via homologous recombination with high targeting efficiency. The targeted clone retained the main pluripotent properties and was differentiated into cardiomyocytes. Significantly, the dystrophin expression and membrane localization were restored in the genetic corrected iPSCs and their derived cardiomyocytes. More importantly, the enhanced spontaneous contraction was observed in modified cardiomyocytes. These results provide a proof of principle for an efficient targeted gene addition for DMD gene therapy and represents a significant step toward precisely therapeutic for DMD. • Site-specific integrated mini-dystrophin into rDNA locus in DMD-iPSCs. • Dystrophin expression and localization were restored in targeted iPSCs and iCMs. • The enhanced spontaneous contraction was observed in the targeted iCMs. [ABSTRACT FROM AUTHOR]

Published

2021

5. Mutation screening of the GLIS3 gene in a cohort of 592 Chinese patients with congenital hypothyroidism.

Author

Fu, Chunyun, Luo, Shiyu, Long, Xigui, Li, Yingfeng, She, Shangyang, Hu, Xuehua, Mo, Meizhen, Wang, Zhanghong, Chen, Yuhua, He, Chun, Su, Jiasun, Zhang, Yue, Lin, Fei, Xie, Bobo, Li, Qifei, and Chen, Shaoke

Subjects

*CONGENITAL hypothyroidism, *GENETIC mutation, *GENETIC testing, *PUBLIC health, *DISEASE prevalence, *GENETICS

Abstract

Objectives Defects in the human GLI-similar 3 ( GLIS3 ) gene are reported to be a rare cause of congenital hypothyroidism (CH) and neonatal diabetes. The aim of this study was to examine the prevalence of GLIS3 mutation among CH patients in the Guangxi Zhuang Autonomous Region of China and to define the relationships between GLIS3 genotypes and clinical phenotypes. Methods Blood samples were collected from 592 patients with CH in Guangxi Zhuang Autonomous Region, China, and genomic DNA was extracted from peripheral blood leukocytes. All exons of the GLIS3 gene with their exon-intron boundaries were screened by next-generation sequencing (NGS) and CNVplex®. Chromosomal microarray analysis (CMA) was performed to detect the existence of the adjacent gene deletion. Results NGS and CNVplex® analysis of GLIS3 in 592 CH patients revealed two different variations in two individuals (2/592, 0.3%). Patient 1 was the paternal allele of 9p24.3p23 heterozygous deletion including the whole GLIS3 gene, and patient 2 was heterozygous for c.2159G > A (p.R720Q) GLIS3 variant combined with compound heterozygous DUOX2 mutations (p.R683L/p.L1343F). Conclusions Our study indicated that the prevalence of GLIS3 variations was 0.3% among studied Chinese CH patients. Multiple variations in one or more CH associated genes can be found in one patient. We found a novel GLIS3 variation c.2159G > A (p.R720Q), thereby expanding the variation spectrum of the gene. [ABSTRACT FROM AUTHOR]

Published

2018

6. Prenatal and early diagnosis of Chinese 3-M syndrome patients with novel pathogenic variants.

Author

Hu, Xuyun, Li, Hongdou, Gui, Baoheng, Xu, Yufei, Wang, Jin, Li, Niu, Su, Jiasun, Zhang, Shujie, Song, Yanning, Wang, Yi, Luo, Jingsi, Fan, Xin, Wang, Jian, Chen, Shaoke, Gong, Chunxiu, and Shen, Yiping

Subjects

*DWARFISM, *PRENATAL diagnosis, *NUCLEOTIDE sequencing, *PHENOTYPES, *GENETIC mutation, *DIAGNOSIS

Abstract

Background 3-M syndrome is a clinically recognizable yet under-diagnosed primordial growth retardation disorder. Molecular testing for CUL7 , OBSL1 or CCDC8 genes can provide confirmed diagnosis for patients at prenatal or early age. So far, the clinical and molecular features of Chinese 3-M syndrome patients have not been reported. Methods In this article, the authors performed prenatal and early diagnosis of Chinese patients with 3-M syndrome by Next-Generation Sequencing. Results The authors reported six unrelated Chinese 3-M syndrome patients. Five of the six patients were diagnosed before two years of age including one prenatal case. The authors identified six novel pathogenic variants and five previously reported pathogenic variants. The authors' clinical evaluations indicated that Chinese 3-M syndrome patients share similar recognizable features as those reported in patients of other ethnic background. The authors noticed some uncommon features in this small cohort of Chinese patients such as delayed motor development at early ages, undelayed bone age and presence of lower eyelid fat pads. Conclusion The authors' study of Chinese 3-M syndrome patients revealed novel mutations and clinical phenotypes. [ABSTRACT FROM AUTHOR]

Published

2017

7. Next-generation sequencing analysis of TSHR in 384 Chinese subclinical congenital hypothyroidism (CH) and CH patients.

Author

Fu, Chunyun, Wang, Jin, Luo, Shiyu, Yang, Qi, Li, Qifei, Zheng, Haiyang, Hu, Xuyun, Su, Jiasun, Zhang, Shujie, Chen, Rongyu, Luo, Jingsi, Zhang, Yue, Shen, Yiping, Wei, Hongwei, Meng, Dahua, Gui, Baoheng, Zeng, Zhangqin, Fan, Xin, and Chen, Shaoke

Subjects

*CONGENITAL hypothyroidism, *SEQUENCE analysis, *HYPOTHYROIDISM diagnosis, *GENETIC mutation, *CHINESE medicine, *DNA mutational analysis

Abstract

Background Defects in the human TSHR gene are reported to be one of the causes of CH due to thyroid dysgenesis, the purpose of this study was to examine the TSHR mutation spectrum and prevalence in congenital hypothyroidism (CH) and subclinical congenital hypothyroidism (SCH) patients in the Guangxi Zhuang Autonomous Region of China and to evaluate the genotype-phenotype correlations. Methods Blood samples were collected from 384 patients including 240 CH and 144 SCH patients in Guangxi, China. Genomic DNA was extracted from peripheral blood leukocytes. All exons of the 11 known CH associated genes including TSHR together with their exon-intron boundaries were screened by next-generation sequencing (NGS). Results NGS analysis of TSHR revealed nine different variants in ten individuals. Six (4.2%) of 144 patients with SCH were found to harbor monoallelic TSHR variants. Four (1.6%) of 240 patients with CH harbored TSHR variants combined with another monoallelic mutation in either DUOX2 or TG gene. The present study identified five novel variants c.1838A > G (p.Y613C), c.1576G > A (p.A526T), c.2087T > G (p.F696C), c.1631G > A (p.G544E) and c.2051C > A (p.A684D) in TSHR , seven known pathogenic variants c.1349G > A (p.R450H), c.326G > A (p.R109Q), c.2066T > G (p.V689G) and c.2272G > A (p.E758K) in TSHR , IVS3 + 2T > G in TG , and c.1588A > T (p.K530X) and c.2635G > A (p.E879K) in DUOX2 . The previously reported hotspot mutation p.R450H was found in only one SCH patient. Conclusion The prevalence of TSHR mutations was 1.6% in CH patients and 4.2% in SCH patients in Guangxi Zhuang Autonomous Region of China. Monoallelic TSHR pathogenic variants were associated with SCH, while TSHR pathogenic variants combined with monoallelic mutations in DUOX2 or TG gene might contribute to CH. Our study expands the TSHR mutation spectrum and provides the best estimation of mutation rate for SCH and CH patients in this Chinese population. [ABSTRACT FROM AUTHOR]

Published

2016

8. Next-generation sequencing analysis of DUOX2 in 192 Chinese subclinical congenital hypothyroidism (SCH) and CH patients.

Author

Fu, Chunyun, Luo, Shiyu, Zhang, Shujie, Wang, Jin, Zheng, Haiyang, Yang, Qi, Xie, Bobo, Hu, Xuyun, Fan, Xin, Luo, Jingsi, Chen, Rongyu, Su, Jiasun, Shen, Yiping, Gu, Xuefan, and Chen, Shaoke

Subjects

*CONGENITAL hypothyroidism, *OXIDASES, *CHINESE people, *GENETIC mutation, *DISEASE prevalence, *BLOOD sampling, *PATIENTS, *DISEASES

Abstract

Background Defects in the human dual oxidase 2 ( DUOX2 ) gene are reported to be one of the major causes of congenital hypothyroidism (CH). This study was set to examine the DUOX2 mutation spectrum and prevalence among Chinese CH and subclinical congenital hypothyroidism (SCH) patients and to define the relationships between DUOX2 genotypes and clinical phenotypes. Methods Peripheral venous blood samples were collected from 192 CH/SCH patients in Guangxi Zhuang Autonomous Region of China. All exons and their exon-intron boundary sequences of the 11 known CH associated genes including DUOX2 were screened by next-generation sequencing (NGS). Results NGS analysis of DUOX2 revealed 18 rare non-polymorphic variants in 57 CH/SCH patients. Sequencing of other CH candidate genes in the 57 patients revealed 2 thyroglobulin ( TG ) variants. All variants included 11 known mutations, 8 novel variants in DUOX2 and one novel variant in TG , among which three variants p.K530X, p.L1343F and p.R683L are highly recurrent in our patient cohort. 35 (83%) of the 42 patients with one or two DUOX2 pathogenic variants turned out to be SCH or transient congenital hypothyroidism (TCH), whereas 13 (87%) of the 15 patients with three or more DUOX2 pathogenic variants are associated with permanent congenital hypothyroidism (PCH). The accumulation of defects in DUOX2 contribute to the more severe disease regarding thyroid stimulating hormone (TSH) levels, free thyroxine (FT4) levels and initial dose of l -thyroxine (L-T4). Conclusion Our study expanded the mutational spectrum of the DUOX2 and TG genes and provided the best estimation of the DUOX2 mutation rate (29%) for CH/SCH patients in Guangxi Zhuang Autonomous Region of China. Most one or two DUOX2 pathogenic variants turned out to be SCH or TCH, whereas patients with three or more DUOX2 pathogenic variants were mostly associated with PCH. The coexistence of multiple pathogenic variants may have contributed to the severity of the hypothyroid condition. [ABSTRACT FROM AUTHOR]

Published

2016

9. Thyroglobulin gene mutations in Chinese patients with congenital hypothyroidism.

Author

Hu, Xuyun, Chen, Rongyu, Fu, Chunyun, Fan, Xin, Wang, Jin, Qian, Jiale, Yi, Shang, Li, Chuan, Luo, Jingsi, Su, Jiasun, Zhang, Shujie, Xie, Bobo, Zheng, Haiyang, Lai, Yunli, Chen, Yun, Li, Hongdou, Gu, Xuefan, Chen, Shaoke, and Shen, Yiping

Subjects

*THYROGLOBULIN, *GENETIC mutation, *CONGENITAL hypothyroidism, *SPECTRUM analysis, *THYRONINES

Abstract

Mutations in Thyroglobulin ( TG ) are common genetic causes of congenital hypothyroidism (CH). But the TG mutation spectrum and its frequency in Chinese CH patients have not been investigated. Here we conducted a genetic screening of TG gene in a cohort of 382 Chinese CH patients. We identified 22 rare non-polymorphic variants including six truncating variants and 16 missense variants of unknown significance (VUS). Seven patients carried homozygous pathogenic variants, and three patients carried homozygous or compound heterozygous VUS. 48 out of 382 patients carried one of 18 heterozygous VUS which is significantly more often than their occurrences in control cohort (P < 0.0001). Unique to Asian population, the c.274+2T>G variant is the most common pathogenic variant with an allele frequency of 0.021. The prevalence of CH due to TG gene defect in Chinese population was estimated to be approximately 1/101,000. Our study uncovered ethnicity specific TG mutation spectrum and frequency. [ABSTRACT FROM AUTHOR]

Published

2016

10. PAX8 pathogenic variants in Chinese patients with congenital hypothyroidism.

Author

Fu, Chunyun, Chen, Rongyu, Zhang, Shujie, Luo, Shiyu, Wang, Jin, Chen, Yun, Zheng, Haiyang, Su, Jiasun, Hu, Xuyun, Fan, Xin, Luo, Jingsi, Yi, Shang, Lai, Yunli, Li, Chuan, Xie, Bobo, Shen, Yiping, Gu, Xuefan, and Chen, Shaoke

Subjects

*CONGENITAL hypothyroidism, *GENETIC mutation, *GENOMICS, *DNA analysis, *LEUCOCYTES, *COHORT analysis

Abstract

Background The clinical presentation of patients with congenital hypothyroidism (CH) caused by paired box gene 8 ( PAX8 ) pathogenic variants is variable and PAX8 mutation rates differ significantly among different populations. This study was set to examine the PAX8 mutation spectrum and prevalence among patients with CH in Guangxi Zhuang Autonomous Region, China. Methods Peripheral venous blood samples were collected from the patients. Genomic DNA was extracted from peripheral blood leukocytes. All exons of the 11 known CH associated genes including PAX8 together with their exon–intron boundaries were screened by next-generation sequencing (NGS). Permanent or transient CH was determined using the results of thyroid function tests after temporary withdrawal of l -thyroxine ( l -T4) therapy at approximately 2 years of age. Results Next generation sequencing analysis of PAX8 in 378 CH patients revealed five different mutations in nine individuals (two are siblings). The mutations included two known missense variants, namely c.92G > A (p.R31H) and c.91C > T (p.R31C), and one novel missense variant c.68G > T (p.G23V), as well as two novel nonsense variants c.1090C > T (p. R364X) and c.658C > T (p.R220X). The variant c.92G > A (p.R31H) is highly recurrent in our patient cohort but the clinical phenotypes vary greatly among those carrying this variant. PAX8 pathogenic variants were mainly associated with permanent CH. Conclusion The prevalence of PAX8 pathogenic variants was 2.38% among patients with CH in Guangxi. Our study expanded the PAX8 mutation spectrum and provided the best estimation of PAX8 mutation rate among CH patients in Guangxi, China. [ABSTRACT FROM AUTHOR]

Published

2015