西班牙患者中LOXL1基因变异及其与假性剥脱性青光眼(XFG)的关联。
LOXL1 gene variants and their association with pseudoexfoliation glaucoma (XFG) in Spanish patients.
作者信息
Álvarez Lydia, García Montserrat, González-Iglesias Héctor, Escribano Julio, Rodríguez-Calvo Pedro P, Fernández-Vega Luis, Coca-Prados Miguel
机构信息
Fundación de Investigación Oftalmológica, Instituto Oftalmológico Fernández-Vega, Avenida Doctores Fernández-Vega, 34, Oviedo, 33012, Spain.
Laboratorio de Genética Molecular Humana, Facultad de Medicina/Instituto de Investigación en Discapacidades Neurológicas (IDINE), Universidad de Castilla-La Mancha, Albacete, 02006, Spain.
出版信息
BMC Med Genet. 2015 Aug 31;16:72. doi: 10.1186/s12881-015-0221-y.
BACKGROUND
LOXL1 gene is the most important genetic risk factor known so far for pseudoexfoliation glaucoma (XFG). Our purpose was to evaluate the potential association of individual genetic variants of the lysyl oxidase-like 1 (LOXL1) gene and haplotypes with XFG in Spanish patients.
METHODS
Blood samples were collected from a total of 105 Spanish patients with XFG and 200 healthy controls. The entire LOXL1 gene along with the promoter, coding and non-coding regions including the 5'- and 3'-untranslated regions, were sequenced using next-generation sequencing in 99 XFG patients. SNPs rs16958477 (promoter), rs1048661 (exon 1), rs3825942 (exon 1), rs2165241 (intron 1) and rs3522 (exon 7) in LOXL1 were genotyped by restriction fragment-length polymorphism (RFLP) in all Spanish control participants and in six additional XFG patients, and a case-control association study was performed. Comparisons of the allelic and genotypic frequencies were performed using standard χ(2) test with Bonferroni and Pearson corrections. Logistic regression analyses were permormed using Sigmaplot v11. Haplotypes frequencies were performed using HaploView 4.0.
RESULTS
Sequencing of the LOXL1 gene in XFG participants identified a total of 212 SNPs, of which 49 exhibited allelic frequencies with significant differences between cases and controls, and 66 were not previously described. The allele frequencies of SNPs rs16958477, rs1048661, rs3825942, rs2165241, were significantly associated with an increased risk for XFG, however the SNP rs3522 was not. The haplotype frequencies of SNPs rs16958477, rs1048661, rs3825942 and rs2165241 and their association with XFG indicated that the CGGT haplotype, containing all four risk alleles, and the AGGT haplotype, which carries the protective allele of rs16958477 and three risk alleles of the other three SNPs, were significantly associated with XFG (p = 4.5×10(-6), and p = 8.8×10(-6)), conferring more than 2-fold increased disease susceptibility.
CONCLUSIONS
SNPs of the LOXL1 gene are associated with XFG in the Spanish population. This information adds new support to the distinct risk association frequencies of LOXL1 alleles with XFG in Western European and Asian populations. Identification and validation of additional SNPs along the entire LOXL1 gene of XFG cases may provide insightful information on their potential role in the pathogenesis of this disease.
背景
赖氨酰氧化酶样1(LOXL1)基因是目前已知的剥脱性青光眼(XFG)最重要的遗传风险因素。我们的目的是评估西班牙患者中赖氨酰氧化酶样1(LOXL1)基因的个体遗传变异和单倍型与XFG的潜在关联。
方法
共收集了105名西班牙XFG患者和200名健康对照者的血样。使用下一代测序技术对99名XFG患者的整个LOXL1基因及其启动子、编码区和非编码区(包括5'和3'非翻译区)进行测序。通过限制性片段长度多态性(RFLP)对所有西班牙对照参与者和另外6名XFG患者的LOXL1基因中的单核苷酸多态性(SNP)rs16958477(启动子)、rs1048661(外显子1)、rs3825942(外显子1)、rs2165241(内含子1)和rs3522(外显子7)进行基因分型,并进行病例对照关联研究。使用标准χ²检验并进行Bonferroni和Pearson校正来比较等位基因和基因型频率。使用Sigmaplot v11进行逻辑回归分析。使用HaploView 4.0计算单倍型频率。
结果
对XFG参与者的LOXL1基因进行测序共鉴定出212个SNP,其中49个SNP的等位基因频率在病例组和对照组之间存在显著差异,66个SNP此前未被描述。SNP rs16958477、rs1048661、rs3825942、rs2165241的等位基因频率与XFG风险增加显著相关,然而SNP rs3522并非如此。SNP rs16958477、rs1048661、rs3825942和rs2165241的单倍型频率及其与XFG的关联表明,包含所有四个风险等位基因的CGGT单倍型以及携带rs16958477的保护性等位基因和其他三个SNP的三个风险等位基因的AGGT单倍型与XFG显著相关(p = 4.5×10⁻⁶和p = 8.8×10⁻⁶),使疾病易感性增加了两倍多。
结论
LOXL1基因的SNP与西班牙人群中的XFG相关。这一信息为西欧和亚洲人群中LOXL1等位基因与XFG的不同风险关联频率提供了新的支持。对XFG病例的整个LOXL1基因中其他SNP的鉴定和验证可能会为它们在该疾病发病机制中的潜在作用提供有价值的信息。
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