Rare Complement Factor H Variant Associated With Age-Related Macular Degeneration in the Amish

被引:40
|
作者
Hoffman, Joshua D. [1 ]
Bailey, Jessica N. Cooke [2 ]
D'Aoust, Laura [1 ]
Cade, William [3 ]
Ayala-Haedo, Juan [3 ]
Fuzzell, Denise [2 ]
Laux, Renee [2 ]
Adams, Larry D. [3 ]
Reinhart-Mercer, Lori [3 ]
Caywood, Laura [3 ]
Whitehead-Gay, Patrice [3 ]
Agarwal, Anita [4 ]
Wang, Gaofeng [3 ]
Scott, William K. [3 ]
Pericak-Vance, Margaret A. [3 ]
Haines, Jonathan L. [1 ,2 ]
机构
[1] Vanderbilt Univ, Med Ctr, Ctr Human Genet Res, Nashville, TN USA
[2] Case Western Reserve Univ, Dept Epidemiol & Biostat, Cleveland, OH 44106 USA
[3] Univ Miami, Miller Sch Med, John P Hussman Inst Human Genom, Miami, FL 33136 USA
[4] Vanderbilt Univ, Dept Ophthalmol & Visual Sci, Nashville, TN 37235 USA
基金
美国国家卫生研究院;
关键词
age-related macular degeneration; linkage analysis; rare variant; exome sequencing; risk score analysis; AMERICAN ANABAPTIST GENEALOGY; LINKAGE ANALYSIS; CHROMOSOME; 10Q26; HIGH-RISK; GENE; MACULOPATHY; PREVALENCE; IDENTIFICATION; POPULATION; LOC387715;
D O I
10.1167/iovs.13-13684
中图分类号
R77 [眼科学];
学科分类号
100212 ;
摘要
PURPOSE. Age-related macular degeneration is the leading cause of blindness among the adult population in the developed world. To further the understanding of this disease, we have studied the genetically isolated Amish population of Ohio and Indiana. METHODS. Cumulative genetic risk scores were calculated using the 19 known allelic associations. Exome sequencing was performed in three members of a small Amish family with AMD who lacked the common risk alleles in complement factor H (CFH) and ARMS2/HTRA1. Follow-up genotyping and association analysis was performed in a cohort of 973 Amish individuals, including 95 with self-reported AMD. RESULTS. The cumulative genetic risk score analysis generated a mean genetic risk score of 1.12 (95% confidence interval [CI]: 1.10, 1.13) in the Amish controls and 1.18 (95% CI: 1.13, 1.22) in the Amish cases. This mean difference in genetic risk scores is statistically significant (P = 0.0042). Exome sequencing identified a rare variant (P503A) in CFH. Association analysis in the remainder of the Amish sample revealed that the P503A variant is significantly associated with AMD (P = 9.27 X 10(-13)). Variant P503A was absent when evaluated in a cohort of 791 elderly non-Amish controls, and 1456 non-Amish cases. CONCLUSIONS. Data from the cumulative genetic risk score analysis suggests that the variants reported by the AMDGene consortium account for a smaller genetic burden of disease in the Amish compared with the non-Amish Caucasian population. Using exome sequencing data, we identified a novel missense mutation that is shared among a densely affected nuclear Amish family and located in a gene that has been previously implicated in AMD risk.
引用
收藏
页码:4455 / 4460
页数:6
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