Molecular Characterization and Ophthalmic Investigation of a Large Family With Type 2A von Hippel-Lindau Disease

doi:10.1001/archopht.119.11.1659

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Vol. 119 No. 11, November 2001

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Ophthalmic Molecular Genetics

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Molecular Characterization and Ophthalmic Investigation of a Large Family With Type 2A von Hippel–Lindau Disease

Richard C. Allen, MD, PhD; Andrew R. Webster, MA, FRCOphth, MD; Ruifang Sui, MD; Jeremiah Brown, MD, MS; Christine M. Taylor, BS; Edwin M. Stone, MD, PhD

Arch Ophthalmol. 2001;119:1659-1665.

Background Von Hippel–Lindau (VHL) disease is adominantly inherited cancer syndrome. Since the identificationof the VHL gene, at least 3 clinical-genetic subtypes of thedisease have been recognized.

Objectives To identify the specific abnormality in theVHL gene and to correlate it with the prevalence and severityof ocular involvement in a large family with VHL disease.

Methods A longitudinal clinical study and DNA analysisof 24 family members.

Results All 14 affected family members exhibited a thymine-to-cysteinechange at nucleotide 505 (T505C) in exon 1 of the VHL gene,consistent with the clinical diagnosis of VHL disease subtype2A. Two asymptomatic gene carriers were also identified. Seventy-fivepercent (12/16) of the gene carriers had 1 or more ocular angiomas.The mean number of ocular angiomas per gene carrier was 3.3.Six eyes had optic disc angioma. Five gene carriers (31%) hadlost vision because of angiomatosis. Cerebellar hemangioblastomaswere present in 4 patients (25%) and pheochromocytomas in 11(69%). No patient was found to have a renal cell carcinoma.

Conclusions The family shows a low susceptibility to renalcarcinoma consistent with the clinical diagnosis of VHL diseasetype 2A. The prevalence and severity of ocular angiomatosisin this subtype do not significantly differ from those of theother more common subtypes of VHL. Recognition of the VHL disease2A phenotype suggests the presence of a specific mutation (T505C)in the VHL gene. Confirmation of this genotype increases theclinician's ability to provide favorable prognostic informationto affected family members.

From the Cullen Eye Institute, Baylor College of Medicine, Houston, Tex (Dr Allen); Moorfields Eye Hospital, London, England (Dr Webster); Department of Ophthalmology and Visual Sciences, The University of Iowa College of Medicine, Iowa City (Drs Sui and Stone and Ms Taylor); and Walter Reed Army Institute of Research, San Antonio, Tex (Dr Brown).

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