Clinical and Genetic Investigation of a Multi-generational Chinese Family Afflicted with Von Hippel-Lindau Disease

Overview

Journal Chin Med J (Engl)

Specialty General Medicine

Date 2015 Jan 8

PMID 25563310

Citations 4

Authors

Jingyao Zhang

Jie Ma

Xiaoyun Du

Dapeng Wu

Hong Ai

Jigang Bai

Shunbin Dong

Qinling Yang

Kai Qu

Yi Lyu

Robert K Valenzuela

Chang Liu

Affiliations

Soon will be listed here.

Abstract

Background: Von Hippel-Lindau (VHL) disease is a hereditary tumor disorder caused by mutations or deletions of the VHL gene. Few studies have documented the clinical phenotype and genetic basis of the occurrence of VHL disease in China. This study armed to present clinical and genetic analyses of VHL within a five-generation VHL family from Northwestern China, and summarize the VHL mutations and clinical characteristics of Chinese families with VHL according to previous studies.

Methods: An epidemiological investigation of family members was done to collect the general information. A retrospective study of clinical VHL cases was launched to collect the relative clinical data. Genetic linkage and haplotype analysis were used to make sure the linkage of VHL to disease in this family. The VHL gene screening was performed by directly analyzing DNA sequence output. At last, we summarized the VHL gene mutation in China by the literature review.

Results: A five-generation North-western Chinese family afflicted with VHL disease was traced in this research. The family consisted of 38 living family members, of whom nine were affected. The individuals afflicted with VHL exhibited multi-organ tumors that included pheochromocytomas (8), central nervous system hemangioblastomas (3), pancreatic endocrine tumors (2), pancreatic cysts (3), renal cysts (4), and paragangliomas (2). A linkage analysis resulted in a high maximal LOD score of 8.26 (theta = 0.0) for the marker D3S1263, which is in the same chromosome region as VHL. Sequence analysis resulted in the identiﬁcation of a functional C>T transition mutation (c. 499 C>T, p.R167W) located in exon 3 of the 167 th codon of VHL. All affected individuals shared this mutation, whereas the unaffected family members and an additional 100 unrelated healthy individuals did not. To date, 49 mutations have been associated with this disease in Chinese populations. The most frequent VHL mutations in China are p.S65 W, p.N78 S, p.R161Q and p.R167 W.

Conclusions: The results supported the notion that the genomic sequence that corresponds to the 167 th residue of VHL is a mutational hotspot. Further research is needed to clarify the molecular role of VHL in the development of organ-specific tumors.

Citing Articles

VHL syndrome without clear family history: A rare case report and literature review of Chinese patients.

Li Y, Xin X, Song W, Zhang X, Chen S, Wang Q Front Neurol. 2022; 13:951054.

PMID: 36324386 PMC: 9618664. DOI: 10.3389/fneur.2022.951054.

Novel gene mutation in von Hippel-Lindau disease - a report of two cases.

Wang J, Cao W, Wang Z, Zhu H BMC Med Genet. 2019; 20(1):194.

PMID: 31823746 PMC: 6902464. DOI: 10.1186/s12881-019-0930-8.

Unsuspected Von Hippel-Lindau syndrome in acute-onset resistant hypertension.

Sivaskandarajah G, Arnason T BMJ Case Rep. 2018; 2018.

PMID: 30042107 PMC: 6059227. DOI: 10.1136/bcr-2018-225162.

A pediatric case of pheochromocytoma without apparent hypertension associated with von Hippel-Lindau disease.

Igaki J, Nishi A, Sato T, Hasegawa T Clin Pediatr Endocrinol. 2018; 27(2):87-93.

PMID: 29662268 PMC: 5897584. DOI: 10.1297/cpe.27.87.

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