Kaur Inderjeet, Hussain Avid, Hussain Nazimul, Das Taraprasad, Pathangay Avinash, Mathai Annie, Hussain Anjli, Nutheti Rishita, Nirmalan Praveen K, Chakrabarti Subhabrata
Kallam Anji Reddy Molecular Genetics Laboratory, Hyderabad, India.
Invest Ophthalmol Vis Sci. 2006 Sep;47(9):3729-35. doi: 10.1167/iovs.05-1430.
To screen polymorphisms in complement factor-H (CFH), toll-like receptor 4 (TLR4), and APOE genes as potential risk factors for age-related macular degeneration (AMD) in Indian patients.
One hundred patients with AMD and 120 normal control subjects were screened for the polymorphisms by restriction digestion and resequencing. Five intragenic SNPs in CFH were screened to generate haplotype data in cases and controls. The data were analyzed in conjunction with data from other populations based on genotype and haplotype frequencies, and odds ratios were computed to estimate the risk of AMD in the different genotypes.
Significant association was noted with the CFH variant (Tyr402His) among AMD cases (P = 1.19 x 10(-7)). Individuals homozygous for the mutant genotype CC had a significantly higher risk (P < 0.0001) of AMD (OR = 11.52; 95% CI 5.05-26.28) than those carrying a single copy of the C allele (OR = 1.51; 95% CI 0.82-2.80), after adjusting for age, gender, and diabetes. Linkage disequilibrium and haplotype analysis at the CFH locus indicated the C-G-T-C-A-G to be a risk haplotype (P = 0.0003). No significant differences were observed in the genotype frequencies of APOE polymorphisms among patients and control subjects (P = 0.76). The carriers of epsilon4 allele had a reduced risk (P = 0.03) of AMD (OR = 0.42, 95% CI 0.19-0.91). TLR4 did not exhibit any association with AMD.
The CFH polymorphism Tyr402His appears indicative of AMD pathogenesis. Diabetes, age, and gender in the presence of the homozygous "CC" genotype in CFH carry an increased risk of AMD. Hence this polymorphism could be used as a potential marker for predictive testing across continents.
筛查补体因子H(CFH)、Toll样受体4(TLR4)和载脂蛋白E(APOE)基因的多态性,以确定其作为印度年龄相关性黄斑变性(AMD)患者潜在危险因素的可能性。
通过限制性酶切和重测序对100例AMD患者和120名正常对照者进行多态性筛查。对CFH基因中的5个基因内单核苷酸多态性(SNP)进行筛查,以生成病例组和对照组的单倍型数据。基于基因型和单倍型频率,结合其他人群的数据对这些数据进行分析,并计算优势比以评估不同基因型中AMD的风险。
在AMD病例中,CFH变异体(Tyr402His)存在显著关联(P = 1.19×10⁻⁷)。在调整年龄、性别和糖尿病因素后,纯合突变基因型CC的个体患AMD的风险显著更高(P < 0.0001)(OR = 11.52;95%置信区间5.05 - 26.28),高于携带单个C等位基因的个体(OR = 1.51;95%置信区间0.82 - 2.80)。CFH基因座的连锁不平衡和单倍型分析表明,C - G - T - C - A - G是一个风险单倍型(P = 0.0003)。患者和对照者中APOE多态性的基因型频率未观察到显著差异(P = 0.76)。携带ε4等位基因的个体患AMD的风险降低(P = 0.03)(OR = 0.42,95%置信区间0.19 - 0.91)。TLR4与AMD未表现出任何关联。
CFH多态性Tyr402His似乎可指示AMD的发病机制。在CFH基因中存在纯合“CC”基因型的情况下,糖尿病、年龄和性别会增加患AMD的风险。因此,这种多态性可作为跨大陆预测性检测的潜在标志物。