Your search keyword '"Zhang, Victor Wei"' showing total 6 results

1. Identification and Functional Characterization of a Novel Nonsense Variant in ARR3 in a Southern Chinese Family With High Myopia.

Author

Yuan, Dejian, Yan, Tizhen, Luo, Shiqiang, Huang, Jun, Tan, Jianqiang, Zhang, Jianping, Zhang, Victor Wei, Lan, Yueyuan, Hu, Taobo, Guo, Jing, Huang, Mingwei, and Zeng, Dingyuan

Subjects

MYOPIA, GENETIC counseling, PRENATAL diagnosis, GENETIC mutation, PHENOTYPES

Abstract

ARR3 has been associated with X-linked, female-limited, high myopia. However, using exome sequencing (ES), we identified the first high myopia case with hemizygous ARR3 -related mutation in a male patient in a Southern Chinese family. This novel truncated mutation (ARR3 : c.569C>G, p.S190*) co-segregated with the disease phenotype in affected family members and demonstrated that high myopia caused by ARR3 is not X-linked, female-limited, where a complicated X-linked inheritance pattern may exist. Thus, our case expanded the variant spectrum in ARR3 and provided additional information for genetic counseling, prenatal testing, and diagnosis. Moreover, we characterized the nonsense-mediated decay of the ARR3 mutant mRNA and discussed the possible underlying pathogenic mechanisms. [ABSTRACT FROM AUTHOR]

Published

2021

2. Novel Mutations in the GTPBP3 Gene for Mitochondrial Disease and Characteristics of Related Phenotypic Spectrum: The First Three Cases From China.

Author

Yan, Hui-ming, Liu, Zhi-mei, Cao, Bei, Zhang, Victor Wei, He, Yi-duo, Jia, Zheng-jun, Xi, Hui, Liu, Jing, Fang, Fang, and Wang, Hua

Subjects

PHENOTYPES, GENETIC mutation, MITOCHONDRIA, GENETIC counseling, OXIDATIVE phosphorylation, MITOCHONDRIAL DNA abnormalities, MISSENSE mutation

Abstract

Combined Oxidative Phosphorylation Deficiency 23 (COXPD23) caused by mutations in GTPBP3 gene is a rare mitochondrial disease, and this disorder identified from the Chinese population has not been described thus far. Here, we report a case series of three patients with COXPD23 caused by GTPBP3 mutations, from a severe to a mild phenotype. The main clinical features of these patients include lactic acidosis, myocardial damage, and neurologic symptoms. Whole genome sequencing and targeted panels of candidate human mitochondrial genome revealed that patient 1 was a compound heterozygote with novel mutations c.413C > T (p. A138V) and c.509_510del (p. E170Gfs∗42) in GTPBP3. Patient 2 was a compound heterozygote with novel mutations c.544G > T (p. G182X) and c.785A > C (p.Q262P), while patient 3 was a compound heterozygote with a previously reported mutation c.424G > A (p.E142K) and novel mutation c.785A > C (p.Q262P). In conclusion, we first describe three Chinese individuals with COXPD23, and discuss the genotype-phenotype correlations of GTPBP3 mutations. Our findings provide novel information in the diagnosis and genetic counseling of patients with mitochondrial disease. [ABSTRACT FROM AUTHOR]

Published

2021

3. Autosomal dominant tubulointerstitial kidney disease genotype and phenotype correlation in a Chinese cohort.

Author

Gong, Kunjing, Xia, Min, Wang, Yaqin, Wang, Na, Liu, Ying, Zhang, Victor Wei, Cheng, Hong, and Chen, Yuqing

Subjects

TUBULOINTERSTITIAL nephritis & uveitis syndrome, KIDNEY diseases, PHENOTYPES, CHINESE people, DNA copy number variations, FOLLOW-up studies (Medicine)

Abstract

Genes of UMOD, HNF1B, MUC1, REN and SEC61A1 were reported to be associated with autosomal dominant tubulointerstitial kidney disease (ADTKD). 48 probands and their family members (N = 27) were enrolled in this genetic screening study. A combination of methods was employed for comprehensive molecular analysis of both copy number variations (CNVs) and single nucleotide variants (SNVs). 35 probands were followed for years. The phenotype-genotype and genotype-outcome correlation were inferred from these datasets. In this cohort, 18 probands were diagnosed with ADTKD, according to Kidney Disease: Improving Global Outcomes (KDIGO) guideline. Moreover, 11 probands were diagnosed with ADTKD-UMOD, one with ADTKD-REN and one with ADTKD-HNF1B, based on molecularly confirmed pathogenic variants. The 11 UMOD variants were mainly located in codons 28 to 289 and half of the variants were found to change the cysteine amino acid. According to the follow-up data, suspected ADTKD individuals had a better prognosis compared to ADTKD individuals (p = 0.029). Individuals with a cysteine substitution in the UMOD gene appeared to have a better prognosis than individuals with other amino acid substitutions (p = 0.015). [ABSTRACT FROM AUTHOR]

Published

2021

4. Identification of a novel DNMT1 mutation in a Chinese patient with hereditary sensory and autonomic neuropathy type IE.

Author

Wenxia Zheng, Zhenxing Yan, Rongni He, Yaowei Huang, Aiqun Lin, Wei Huang, Yuying Su, Shaoyuan Li, Victor Wei Zhang, Huifang Xie, Zheng, Wenxia, Yan, Zhenxing, He, Rongni, Huang, Yaowei, Lin, Aiqun, Huang, Wei, Su, Yuying, Li, Shaoyuan, Zhang, Victor Wei, and Xie, Huifang

Subjects

GENETIC mutation, DNA methylation, DNA methyltransferases, EMBRYOLOGY, PHENOTYPES, NEUROPATHY

Abstract

Background: DNA methyltransferase 1 (EC 2.1.1.37), encoded by DNMT1 gene, is one of key enzymes in maintaining DNA methylation patterns of the human genome. It plays a crucial role in embryonic development, imprinting and genome stability, cell differentiation. The dysfunction of this group of enzymes can lead to a variety of human genetic disorders. Until now, mutations in DNMT1 have been found to be associated with two distinct phenotypes. Mutations in exon 20 of this gene leads to hereditary sensory and autonomic neuropathy type IE, and mutations in exon 21 cause autosomal dominant cerebellar ataxia, deafness and narcolepsy.Case Presentation: Here we report a novel DNMT1 mutation in a sporadic case of a Chinese patient with cerebellar ataxia, multiple motor and sensory neuropathy, hearing loss and psychiatric manifestations. Furthermore, we elucidated its pathogenic effect through molecular genetics studies and revealed that this defective DNMT1 function is responsible for the phenotypes in this individual.Conclusion: Our findings expand the spectrum of DNMT1-related disorders and provide a good example of precision medicine through the combination of exome sequencing and clinical testing. [ABSTRACT FROM AUTHOR]

Published

2018

5. Genetic evidence of 'genuine' empty follicle syndrome: a novel effective mutation in the LHCGR gene and review of the literature.

Author

Ping Yuan, Zuyong He, Lingyan Zheng, Wenjun Wang, Yu Li, Haijing Zhao, Victor Wei Zhang, Qingxue Zhang, Dongzi Yang, Yuan, Ping, He, Zuyong, Zheng, Lingyan, Wang, Wenjun, Li, Yu, Zhao, Haijing, Zhang, Victor Wei, Zhang, Qingxue, and Yang, Dongzi

Subjects

GENETIC mutation, OVUM, HUMAN in vitro fertilization, CHORIONIC gonadotropins, PHENOTYPES, AMINO acids, CELL receptors, GENETIC techniques, HUMAN reproductive technology, INFERTILITY, OVARIAN diseases, PROTEINS

Abstract

Empty follicle syndrome (EFS) is a reproductive disorder in which no oocytes are retrieved during IVF. The existence of genuine EFS (GEFS) is still controversial, and to date, only one missense mutation of Luteinizing Hormone/Choriogonadotropin Receptor (LHCGR) has been reported to be associated with this disease. Here, we describe a GEFS patient in a non-consanguineous family from China. A 27-year-old woman presented with a 5-year history of primary infertility and LH resistance-like ovaries of unequal sizes, but with normal levels of circulating LH. In spite of a satisfactory ovarian reserve and response, no oocytes were retrieved after two cycles of IVF. Her condition did not appear to be failure of the hCG injection. It is more likely to be a genetic cause. A novel homozygous mutation in LHCGR gene, c.1345G>A (p.Ala449Thr), was detected in this patient. Each of her parents is heterozygous for this change, and the change was absent from 407 control subjects. Alanine at this amino acid position was highly conserved and replacement of threonine was predicted to disrupt the third transmembrane helix of the rhodopsin-like G protein-coupled receptor domain. Protein localization studies revealed that a portion of the mutant LHCGR protein molecules was retained intracellularly. Signalling studies demonstrated that this mutation had differing effects on the response of LHCGR to hCG or LH at different concentrations. Specifically, at a concentration <1 IU/ml, the mutant was activated by hCG stimulation but partially resistant to LH stimulation; at a higher concentration (>1 IU/ml), the mutant was activated by both hCG and LH. These data suggest that screening for mutations in the LHCGR gene may assist in the diagnosis of patients with GEFS. The literature describing the relationship between phenotype and genotypes in females is reviewed, and possible aetiologies and treatment options for this disease are proposed based on our and other studies. [ABSTRACT FROM AUTHOR]

Published

2017

6. Precision Medicine for Continuing Phenotype Expansion of Human Genetic Diseases.

Author

Yu, Hui and Zhang, Victor Wei

Subjects

*CHRONIC diseases, *MEDICAL genetics, *MOLECULAR diagnosis, *PHENOTYPES, *GENOMICS, *INDIVIDUALIZED medicine, *SEQUENCE analysis, *GENOTYPES, *GENETICS

Abstract

Determining the exact genetic causes for a patient and providing definite molecular diagnoses are core elements of precision medicine. Individualized patient care is often limited by our current knowledge of disease etiologies and commonly used phenotypic-based diagnostic approach. The broad and incompletely understood phenotypic spectrum of a disease and various underlying genetic heterogeneity also present extra challenges to our clinical practice. With the rapid adaptation of new sequence technology in clinical setting for diagnostic purpose, phenotypic expansions of disease spectrum are becoming increasingly common. Understanding the underlying molecular mechanisms will help us to integrate genomic information into the workup of individualized patient care and make better clinical decisions. [ABSTRACT FROM AUTHOR]

Published

2015