Phenotypic variability in a French family with a novel mutation in the BEST1 gene causing multifocal best vitelliform macular dystrophy

Phenotypic variability in a French family with a novel mutation in the BEST1 gene causing multifocal best vitelliform macular dystrophy

To describe genetic and clinical findings in a French family affected by best vitelliform macular dystrophy (BVMD). We screened eight at-risk members of a family, including a BVMD-affected proband, by direct sequencing of 11 bestrophin-1 (BEST1) exons. Individuals underwent ophthalmic examination an...

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Bibliographic Details
Published in:Molecular vision Vol. 17; pp. 309 - 322
Main Authors: Lacassagne, Emmanuelle, Dhuez, Aurore, Rigaudière, Florence, Dansault, Anouk, Vêtu, Christelle, Bigot, Karine, Vieira, Véronique, Puech, Bernard, Defoort-Dhellemmes, Sabine, Abitbol, Marc
Format: Journal Article
Language:English
Published: United States Molecular Vision 29-01-2011
Subjects:
Acuity
Adolescent
Adult
Alleles
Angiography
Best vitelliform macular dystrophy
Bestrophins
Child
Chloride Channels - genetics
Deposits
Electrooculography - methods
Electroretinograms
Electroretinography - methods
Evolution
Exons
Eye Proteins - genetics
Family Health
Female
France
Humans
imaging
Male
Middle Aged
Mutation
Pedigree
Phenotype
Retina
Retina - pathology
retinal degeneration
Sequence Analysis, DNA
Tomography
Tomography, Optical Coherence - methods
Vision
visual field
Vitelliform Macular Dystrophy - genetics
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Summary:To describe genetic and clinical findings in a French family affected by best vitelliform macular dystrophy (BVMD). We screened eight at-risk members of a family, including a BVMD-affected proband, by direct sequencing of 11 bestrophin-1 (BEST1) exons. Individuals underwent ophthalmic examination and autofluorescent fundus imaging, indocyanine green angiography, electro-oculogram (EOG), electroretinogram (ERG), multifocal ERG, optical coherence tomography (OCT), and where possible, spectral domain OCT. The sequence analysis of the BEST1 gene revealed one previously unknown mutation, c.15C>A (p.Y5X), in two family members and one recently described mutation, c.430A>G (p.S144G), in five family members. Fundus examination and electrophysiological responses provided no evidence of the disease in the patient carrying only the p.Y5X mutation. Three patients with the p.S144G mutation did not show any preclinical sign of BVMD except altered EOGs. Two individuals of the family exhibited a particularly severe phenotype of multifocal BVMD-one individual carrying the p.S144G mutation heterozygously and one individual harboring both BEST1 mutations (p.S144G inherited from his mother and p.Y5X from his father). Both of these family members had multifocal vitelliform autofluorescent lesions combined with abnormal EOG, and the spectral domain OCT displayed a serous retinal detachment. In addition, ERGs demonstrated widespread retinal degeneration and multifocal ERGs showed a reduction in the central retina function, which could be correlated with the decreased visual acuity and visual field scotomas. A thorough clinical evaluation found no pathological phenotype in the patient carrying the isolated p.Y5X mutation. The patients carrying the p.S144G variation in the protein exhibited considerable intrafamilial phenotypic variability. Two young affected patients in this family exhibited an early onset, severe, multifocal BVMD with a diffuse distribution of autofluorescent deposits throughout the retina and rapid evolution toward the loss of central vision. The other genetically affected relatives had only abnormal EOGs and displayed no or extremely slow electrophysiological evolution.
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ISSN:1090-0535
1090-0535