中介分析以了解习惯性咖啡摄入与痛风之间的遗传关系。
Mediation analysis to understand genetic relationships between habitual coffee intake and gout.
机构信息
Department of Medicine, Faculty of Medical and Health Sciences, University of Auckland, 85 Park Rd, Grafton, Auckland, New Zealand.
Department of Biochemistry, University of Otago, Dunedin, New Zealand.
出版信息
Arthritis Res Ther. 2018 Jul 5;20(1):135. doi: 10.1186/s13075-018-1629-5.
BACKGROUND
Increased coffee intake is associated with reduced serum urate concentrations and lower risk of gout. Specific alleles of the GCKR, ABCG2, MLXIPL, and CYP1A2 genes have been associated with both reduced coffee intake and increased serum urate in separate genome-wide association studies (GWAS). The aim of this study was to determine whether these single nucleotide polymorphisms (SNPs) influence the risk of gout through their effects on coffee consumption.
METHODS
This research was conducted using the UK Biobank Resource. Data were available for 130,966 European participants aged 40-69 years. Gout status and coffee intake were tested for association with four urate-associated SNPs: GCKR (rs1260326), ABCG2 (rs2231142), MLXIPL (rs1178977), and CYP1A2 (rs2472297). Multiple regression and path analysis were used to examine whether coffee consumption mediated the effect of the SNPs on gout risk.
RESULTS
Coffee consumption was inversely associated with gout (multivariate adjusted odds ratio (95% confidence interval (CI)) for any coffee consumption 0.75 (0.67-0.84, P = 9 × 10)). There was also evidence of a dose-effect with multivariate adjusted odds ratio (95% CI) per cup consumed per day of 0.85 (0.82-0.87, P = 9 × 10). The urate-increasing GCKR, ABCG2, MLXIPL, and CYP1A2 alleles were associated with reduced daily coffee consumption, with the strongest associations for CYP1A2 (beta -0.30, P = 8 × 10), and MLXIPL (beta -0.17, P = 3 × 10), and weaker associations for GCKR (beta -0.07, P = 3 × 10) and ABCG2 (beta -0.09, P = 2 × 10). The urate-increasing GCKR and ABCG2 alleles were associated with gout (multivariate adjusted p < 5 × 10 for both), but the urate-increasing MLXIPL and CYP1A2 alleles were not. In mediation analysis, the direct effects of GCKR and ABCG2 accounted for most of the total effect on gout risk, with much smaller indirect effects mediated by coffee consumption.
CONCLUSION
Coffee consumption is inversely associated with risk of gout. Although alleles at several SNPs associate with both lower coffee consumption and higher risk of gout, these SNPs largely influence gout risk directly, rather than indirectly through effects on coffee consumption.
背景
增加咖啡摄入量与血清尿酸浓度降低和痛风风险降低有关。在单独的全基因组关联研究(GWAS)中,GCKR、ABCG2、MLXIPL 和 CYP1A2 基因的特定等位基因与咖啡摄入量减少和血清尿酸升高均有关。本研究的目的是确定这些单核苷酸多态性(SNP)是否通过对咖啡摄入量的影响来影响痛风的风险。
方法
本研究使用 UK Biobank 资源进行。共有 130966 名年龄在 40-69 岁的欧洲参与者的数据可用。测试了痛风状况和咖啡摄入量与四个尿酸相关 SNP 的关联:GCKR(rs1260326)、ABCG2(rs2231142)、MLXIPL(rs1178977)和 CYP1A2(rs2472297)。多元回归和路径分析用于检查咖啡消耗是否介导了 SNP 对痛风风险的影响。
结果
咖啡消耗与痛风呈负相关(任何咖啡消耗的多变量调整比值比(95%置信区间(CI))为 0.75(0.67-0.84,P = 9×10))。每天每多消耗一杯咖啡,多变量调整比值比(95%CI)也有证据表明存在剂量效应,为 0.85(0.82-0.87,P = 9×10)。尿酸升高的 GCKR、ABCG2、MLXIPL 和 CYP1A2 等位基因与每日咖啡消耗减少有关,其中 CYP1A2 的关联最强(β-0.30,P = 8×10),MLXIPL(β-0.17,P = 3×10),GCKR 较弱(β-0.07,P = 3×10)和 ABCG2(β-0.09,P = 2×10)。尿酸升高的 GCKR 和 ABCG2 等位基因与痛风有关(两者的多变量调整 p<5×10),但尿酸升高的 MLXIPL 和 CYP1A2 等位基因则没有。在中介分析中,GCKR 和 ABCG2 的直接效应解释了痛风风险总效应的大部分,而通过咖啡消耗介导的间接效应则小得多。
结论
咖啡消耗与痛风风险呈负相关。尽管一些 SNP 的等位基因与咖啡摄入量减少和痛风风险增加均有关,但这些 SNP 主要通过对咖啡消耗的直接影响而不是通过对咖啡消耗的间接影响来影响痛风风险。
Zotero 插件