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补体因子H 402H变异体与网状黄斑疾病。

Complement factor H 402H variant and reticular macular disease.

作者信息

Smith R Theodore, Merriam Joanna E, Sohrab Mahsa A, Pumariega Nicole M, Barile Gaetano, Blonska Anna M, Haans Raymond, Madigan David, Allikmets Rando

机构信息

Department of Ophthalmology, Harkness Eye Institute, New York, NY 10032, USA.

出版信息

Arch Ophthalmol. 2011 Aug;129(8):1061-6. doi: 10.1001/archophthalmol.2011.212.

Abstract

OBJECTIVE

To determine the association of high-risk alleles in the complement factor H (CFH; Y402H, rs1061170) and age-related maculopathy susceptibility (ARMS2; A69S, rs10490924) genes with reticular macular disease (RMD), a major clinical subphenotype of age-related macular degeneration (AMD).

METHODS

Using retinal images from the Columbia Macular Genetics Study, we identified 67 subject individuals with RMD. A comparison group of 64 subjects with AMD without RMD was matched by ethnicity, age, sex, and AMD clinical stage.

RESULTS

In the RMD group, 53 of 67 subjects (79.1%) were female, the mean age was 83 years, and 47 of 67 (70.1%) had late AMD, with closely matched values in the non-RMD group. The frequencies of the CFH 402H allele were 39.6% in the RMD group (53 of 134 individuals) and 58.6% in the non-RMD group (75 of 128 individuals) (χ(2) = 8.8; P = .003; odds ratio, 0.46 [95% confidence interval, 0.28-0.76]). The corresponding frequencies of the risk allele for ARMS2 were 44.0% (40 of 128 individuals) and 31.3% (40 of 128 individuals), respectively (χ(2) = 4.0; P = .045; odds ratio, 1.73 [95% confidence interval, 1.04-2.90]). Homozygosity for 402H was particularly associated with the absence of RMD, occurring in 8 of 67 subjects (11.9%) with RMD vs 24 of 64 subjects (37.5%) without RMD (P < .001). Retinal macular disease also was associated with hypertension among male patients.

CONCLUSIONS

The AMD-associated CFH 402H risk variant is significantly associated with the absence of RMD but enhanced risk for RMD is conferred by the ARMS2 69S AMD risk allele. These results are consistent with the hypothesis that 402H may confer a survival benefit against certain infections, some of which may cause RMD.

CLINICAL RELEVANCE

Reticular macular disease may be genetically distinct from the rest of AMD.

摘要

目的

确定补体因子H(CFH;Y402H,rs1061170)和年龄相关性黄斑病变易感性(ARMS2;A69S,rs10490924)基因中的高危等位基因与网状黄斑疾病(RMD)的关联,RMD是年龄相关性黄斑变性(AMD)的一种主要临床亚表型。

方法

利用哥伦比亚黄斑遗传学研究的视网膜图像,我们确定了67例患有RMD的受试者个体。选取64例无RMD的AMD受试者作为对照组,根据种族、年龄、性别和AMD临床分期进行匹配。

结果

在RMD组中,67例受试者中有53例(79.1%)为女性,平均年龄为83岁,67例中有47例(70.1%)患有晚期AMD,非RMD组的数值与之相近。CFH 402H等位基因频率在RMD组中为39.6%(134例个体中的53例),在非RMD组中为58.6%(128例个体中的75例)(χ² = 8.8;P = .003;优势比,0.46 [95%置信区间,0.28 - 0.76])。ARMS2风险等位基因的相应频率分别为44.0%(128例个体中的40例)和31.3%(128例个体中的40例)(χ² = 4.0;P = .045;优势比,1.73 [95%置信区间,1.04 - 2.90])。402H纯合子尤其与无RMD相关,在67例患有RMD的受试者中有8例(11.9%)出现,而在64例无RMD的受试者中有24例(37.5%)出现(P < .001)。视网膜黄斑疾病在男性患者中也与高血压相关。

结论

与AMD相关的CFH 402H风险变异与无RMD显著相关,但ARMS2 69S AMD风险等位基因会增加RMD的风险。这些结果与402H可能赋予针对某些感染的生存益处的假设一致,其中一些感染可能导致RMD。

临床意义

网状黄斑疾病在基因方面可能与AMD的其他类型不同。

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