A nonsense mutation in VHL causing Von Hippel-Lindau syndrome in a large Chinese family—a genetic study of familial neoplastic disease

A nonsense mutation in VHL causing Von Hippel-Lindau syndrome in a large Chinese family—a genetic study of familial neoplastic disease

Von Hippel-Lindau (VHL) syndrome is a multi-organ neoplastic disease characterized by highly vascular and cystic tumors in the central nervous system (CNS), retina, and visceral lesions, which are mainly caused by germline mutations in VHL. We aimed to detect novel mutations in VHL gene in families...

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Hauptverfasser: Ding, Xinghuan, Liang, Tingyu, Li, Ben, Liang, Bo, Li, Jingjing, Wang, Fang, Chen, Shichao, Wang, Shanjun, Zheng, Xinmei, Wang, Tongxin, Feng, Enshan
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Biological Sciences not elsewhere classified
Cancer
Chemical Sciences not elsewhere classified
FOS: Biological sciences
FOS: Health sciences
Genetics
Infectious Diseases
Medicine
Molecular Biology
Virology
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creator Ding, Xinghuan
Liang, Tingyu
Li, Ben
Liang, Bo
Li, Jingjing
Wang, Fang
Chen, Shichao
Wang, Shanjun
Zheng, Xinmei
Wang, Tongxin
Feng, Enshan
description Von Hippel-Lindau (VHL) syndrome is a multi-organ neoplastic disease characterized by highly vascular and cystic tumors in the central nervous system (CNS), retina, and visceral lesions, which are mainly caused by germline mutations in VHL. We aimed to detect novel mutations in VHL gene in families with VHL. Here, a large consanguineous four-generation family with variant phenotypes of VHL syndrome was recruited, and its molecular genetics were tested via Sanger sequencing. And various tools and databases were used to predict the variant pathogenicity, frequency, and protein function. Genetic investigation detected a c.351G > A nonsense mutation in VHL that altered the downstream reading frame and created a premature TGA stop signal, resulting in severely truncated pVHL (p.Trp117Ter). This mutation is absent from most public databases, and functional prediction bioinformatic tools demonstrated that this residue is conserved and that this variant is highly likely to be deleterious. The c.315G > A nonsense mutation in VHL is the causal mutation of this kindred that may lead to clear familial aggregation of VHL syndrome because of the dysfunction of the truncated pVHL.
doi_str_mv 10.6084/m9.figshare.24647976
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subjects Biological Sciences not elsewhere classified
Cancer
Chemical Sciences not elsewhere classified
FOS: Biological sciences
FOS: Health sciences
Genetics
Infectious Diseases
Medicine
Molecular Biology
Virology
title A nonsense mutation in VHL causing Von Hippel-Lindau syndrome in a large Chinese family—a genetic study of familial neoplastic disease
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