Frequency of Von Hippel-Lindau Germline Mutations in Classic and Non-classic Von Hippel-Lindau Disease Identified by DNA Sequencing, Southern Blot Analysis and Multiplex Ligation-dependent Probe Amplification

Overview

Journal Clin Genet

Specialty Genetics

Date 2007 Jul 31

PMID 17661816

Citations 28

Authors

F J Hes

R B van der Luijt

A L W Janssen

R A Zewald

G J de Jong

J W Lenders

T P Links

G P M Luyten

R H Sijmons

H J Eussen

D J J Halley

C J M Lips

P L Pearson

A M W van den Ouweland

D F Majoor-Krakauer

Affiliations

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Abstract

The current clinical diagnosis of Von Hippel-Lindau (VHL) disease demands at least one specific [corrected] VHL manifestation in a patient with familial VHL disease, or, in a [corrected] sporadic patient, at least two or more hemangioblastomas or a single hemangioblastoma in combination with a typical visceral lesion. To evaluate this definition, we studied the frequency of germline VHL mutation in three patients groups: (i) multi-organ involvement (classic VHL), (ii) limited VHL manifestations meeting criteria (non-classic VHL) and (iii) patients with VHL-associated tumors not meeting current diagnostic VHL criteria. In addition, we validated multiplex ligation-dependent probe amplification (MLPA) as a rapid and reliable quantitative method for the identification of germline VHL deletions. The frequency of germline VHL mutations was very high in classic VHL cases with multi-organ involvement (95%), lower in non-classic cases that meet current diagnostic criteria but have limited VHL manifestations or single-organ involvement (24%) and low (3.3%), but tangible in cases not meeting current diagnostic VHL criteria. The detection of germline VHL mutations in patients or families with limited VHL manifestations, or single-organ involvement is relevant for follow-up of probands and early identification of at-risk relatives.

Citing Articles

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Genetics, Pathophysiology, and Current Challenges in Von Hippel-Lindau Disease Therapeutics.

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Oldfield L, Grzybowski J, Grenier S, Chao E, Downs G, Farncombe K NPJ Genom Med. 2022; 7(1):21.

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