Clinical features and linkage analysis for a Chinese family with autosomal dominant central areolar choroidal dystrophy.
- Author:
Kai MA
1
;
Xiu-fen YANG
;
Cui HAN
;
Ning ZHANG
;
Jun XU
;
Shou-bin LIU
;
Hai LU
;
Torkel SNELLINGEN
;
Ning-li WANG
;
Ning-pu LIU
Author Information
- Publication Type:Journal Article
- MeSH: Adolescent; Adult; Child; Choroid Diseases; genetics; Electroretinography; Female; Fluorescein Angiography; Genetic Linkage; Humans; Male; Middle Aged
- From: Chinese Medical Journal 2009;122(22):2686-2690
- CountryChina
- Language:English
-
Abstract:
BACKGROUNDA Chinese family with autosomal dominant central areolar choroidal dystrophy (CACD) was identified. The purpose of this study was to collect the clinical findings from the family and to identify the genetic entity by linkage analysis.
METHODSForty-three individuals from 3 generations of the family underwent ophthalmologic examinations, including best-corrected visual acuity, examination of the anterior segments, and inspection of the ocular fundus after pharmacologic mydriasis. Affected family members further underwent color vision test, color fundus photography, fluorescein angiography, automated perimetry, and electroretinography. The family was followed up for 30 months. Peripheral venous blood or buccal swabs were collected from each family member and genomic DNA was extracted. Linkage analysis was performed for candidate genes or loci using microsatellite markers.
RESULTSSeven family members in 3 continuous generations were diagnosed as having autosomal dominant CACD. The family showed progressive development of the disease, affecting both male and female. Age of onset of visual disturbances varied between 11 and 50 years. Phenotypic variability among affected individuals was apparent and ranged from relatively normal-appearing fundus with mild parafoveal pigment mottling to geographic atrophy of the macula. Fluorescein angiography showed hyperfluorescent parafoveal changes in early stage or well-demarcated area of chorioretinal atrophy with enhanced visibility of the residual underlying choroidal vessels in the late stage. Peripheral retina and visual fields were normal in affected individuals. Electroretinogram showed normal or mild reduction in the photopic amplitude. Eight candidate genes (STGD4, RCD1, peripherin/RDS, GUCA1A, RIMS1, UNC119, GUCY2D, and AIPL1) and two genetic loci (4p15.2 - 16.3, and 17p13) were excluded to be responsible for the disease by linkage analysis.
CONCLUSIONSThe clinical findings of this Chinese family with CACD shared similarities with previously reported families of other ethnicities. Linkage analysis excluded the known genes and genetic loci, indicating genetic heterogeneity of the disease.