年龄相关性黄斑变性的常见和罕见遗传风险变异与科英布拉眼病研究中的遗传风险评分。
Common and rare genetic risk variants in age-related macular degeneration and genetic risk score in the Coimbra eye study.
机构信息
AIBILI - Association for Innovation and Biomedical Research on Light and Image, Coimbra, Portugal.
Ophthalmology Department, Coimbra Hospital and Universitary Centre (CHUC), Coimbra, Portugal.
出版信息
Acta Ophthalmol. 2023 Mar;101(2):185-199. doi: 10.1111/aos.15232. Epub 2022 Aug 29.
PURPOSE
To determine the contribution of common and rare genetic variants in age-related macular degeneration (AMD) in a Portuguese population from the Coimbra Eye Study (CES), and the genetic risk score (GRS).
METHODS
Participants underwent ophthalmologic examination and imaging. A centralized reading centre performed AMD staging. Genetic sequencing was carried out with the EYE-RISK assay. Sixty-nine single nucleotide polymorphisms (SNPs) were genotyped and tested for association with AMD. Case-control and progression-to-AMD analyses were performed using logistic regression to assess allelic odds ratio (OR) at a 95% confidence interval (CI) for each variant. GRS was calculated for cases/controls and progressors/non-progressors. Cumulative impact of rare variants was compared between cases/controls using logistic regression.
RESULTS
In case-control analysis (237 cases/640 controls) variants associated with risk of disease were: ARMS2 rs10490924, ARMS2_HTRA1 rs3750846, CFH rs35292876, SLC16A8 rs8135665, TGFBR1 rs1626340. Major risk variants ARMS2/HTRA1 rs3750846, CFH rs570618 and C3 rs2230199 had unexpected lower allele frequency (AF), and the highest risk-conferring variant was a rare variant, CFH rs35292876 (OR, 2.668; p-value = 0.021). In progression-to-AMD analysis (137 progressors/630 non-progressors), variants associated with risk of progression were ARMS2 rs10490924, ARMS2_HTRA1 rs3750846, CFH rs35292876. GRS of cases/controls was 1.124 ± 1.187 and 0.645 ± 1.124 (p-value < 0.001), and of progressors/non-progressors was 1.190 ± 1.178 and 0.669 ± 1.141 (p-value < 0.001). Higher proportion of pathogenic rare CFH variants was observed in cases (OR, 9.661; p-value < 0.001).
CONCLUSIONS
Both common and rare variants were associated with AMD, but a CFH rare variant conferred the highest risk of disease while three major risk variants had a lower-than-expected AF in our population originary from a geographic region with lower prevalence of AMD. GRS was still significantly higher in AMD patients. Damaging CFH rare variants were cumulatively more common in AMD cases.
目的
在科英布拉眼病研究(CES)中,确定葡萄牙人群中与年龄相关性黄斑变性(AMD)相关的常见和罕见遗传变异的贡献,以及遗传风险评分(GRS)。
方法
参与者接受眼科检查和影像学检查。一个集中的阅读中心进行 AMD 分期。使用 EYE-RISK 检测进行基因测序。对 69 个单核苷酸多态性(SNP)进行基因分型,并对其与 AMD 的相关性进行检测。使用逻辑回归对病例对照和进展至 AMD 分析进行分析,以评估每个变异的等位基因比值比(OR)在 95%置信区间(CI)。为病例/对照和进展者/非进展者计算 GRS。使用逻辑回归比较病例/对照之间罕见变异的累积影响。
结果
在病例对照分析(237 例病例/640 例对照)中,与疾病风险相关的变异是:ARMS2 rs10490924、ARMS2_HTRA1 rs3750846、CFH rs35292876、SLC16A8 rs8135665、TGFBR1 rs1626340。主要风险变异 ARMS2/HTRA1 rs3750846、CFH rs570618 和 C3 rs2230199 的等位基因频率(AF)出乎意料地较低,风险最高的变异是罕见变异 CFH rs35292876(OR,2.668;p 值=0.021)。在进展至 AMD 分析(137 例进展者/630 例非进展者)中,与进展风险相关的变异是 ARMS2 rs10490924、ARMS2_HTRA1 rs3750846、CFH rs35292876。病例/对照的 GRS 为 1.124±1.187 和 0.645±1.124(p 值<0.001),进展者/非进展者的 GRS 为 1.190±1.178 和 0.669±1.141(p 值<0.001)。在病例中观察到致病性罕见 CFH 变异的比例更高(OR,9.661;p 值<0.001)。
结论
常见和罕见变异均与 AMD 相关,但 CFH 罕见变异在本研究中,来自 AMD 发病率较低的地理区域的人群中,其疾病风险最高,而三个主要风险变异的 AF 低于预期。AMD 患者的 GRS 仍然显著较高。AMD 病例中累积的破坏性 CFH 罕见变异更为常见。
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