Abstract
Chronic central serous chorioretinopathy (cCSC) is a multifactorial eye disease characterized by subretinal fluid accumulation that leads to vision loss. Clinically, cCSC is associated with stress, hypercortisolism and corticosteroid use, and is more frequent in males (80%) than in females (20%). Current genetic studies on cCSC have thus far focussed on common variants, but familial occurrence of cCSC also suggests a role for rare variants in the disease susceptibility. Therefore, in this study, we performed exome sequencing of cCSC patients to elucidate the role of rare (protein-altering) variants in the disease. Exome sequencing was performed on 269 cCSC patients and 1,586 controls. Data were processed according to the Genome-Analysis-Toolkit (GATK) best practices. Principal component analysis was performed to check for genetic ancestry and only unrelated subjects of European descent were retained. Burden, SKAT and SKAT-O tests were performed using 2 different grouping criteria. One group included protein-altering variants only, while the other contained synonymous and splice site variants as well. The gene-based analyses were performed using the SKAT R-package correcting for two principal components using two approaches; (1) on the entire cohort correcting for sex and (2) on males and females separately. Additionally, the gene-based associations of genes at previously reported cCSC loci were investigated. After filtering, the dataset contained 263 cCSC patients (208 males [79%]) and 1352 controls (671 males [50%]) carrying 197,915 protein-altering variants in 16,370 genes and 330,689 exonic variants in 18,173 genes. Analysis stratified by sex identified significant associations with the PIGZ (PSKAT = 9.19 × 10−7 & PSKAT-O = 2.48 × 10−6), DUOX1 (PSKAT = 1.03 × 10−6), RSAD1 (PSKAT = 1.92 × 10−7 & PSKAT-O = 8.57 × 10−8) and LAMB3 (PBurden = 1.40 × 10−6 & PSKAT-O = 1.14 × 10−6) genes in female cCSC patients, after correction for multiple testing. The number of rare variant carriers in these genes was significantly higher in the female cCSC cohort compared to female controls (45,5% vs. 18.5%, P = 1.92 × 10−6, OR = 3.67 [95% CI = 2.09–6.46]). No significant associations were identified in the entire cohort nor in the male patients. In this exome study on cCSC patients, we have identified PIGZ, DUOX1, RSAD1 and LAMB3 as potential new candidate genes for cCSC in females. The sex-specific associations identified here suggest a possible interaction between rare genetic factors and sex for cCSC, but replication of these findings in additional cohorts of cCSC patients is necessary.
Highlights
Central serous chorioretinopathy (CSC) is a vision-threatening eye disease characterized by serous fluid accumulation between the neuroretina and retinal pigment epithelium (RPE), supposedly secondary to a dysfunctional choroid and outer blood-retina barrier of the RPE1
269 Chronic central serous chorioretinopathy (cCSC) patients and 1586 controls were analysed by exome sequencing
Joint genotyping with GATK resulted in a dataset containing 746,264 single nucleotide polymorphisms (SNPs) and 45,048 INDELs
Summary
Central serous chorioretinopathy (CSC) is a vision-threatening eye disease characterized by serous fluid accumulation between the neuroretina and retinal pigment epithelium (RPE), supposedly secondary to a dysfunctional choroid and outer blood-retina barrier of the RPE1. Www.nature.com/scientificreports was suggested because of familial occurrence of CSC3,4, and so far a limited number of genetic studies have been performed for cCSC. Candidate gene studies have described associations between cCSC and common single nucleotide polymorphisms (SNPs) in the CFH, ARMS2, CDH5 and NR3C2 genes[5,6,7,8], as well as copy number variations (CNVs) of the C4B gene[9]. The first genome-wide association study on cCSC confirmed the role of CFH in the disease[10]. Only common variants have been associated with cCSC, familial clustering of cCSC has hinted towards a possible role for rare variants in disease susceptibility[3,4]. We performed single-variant association and gene-based tests on the entire cohort and by stratifying the analyses for sex. We report new potential candidate genes for cCSC in females, and further broaden our knowledge on the disease etiology
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