Genetically Proxied Antidiabetic Drug Target and Primary Open-Angle Glaucoma: A Mendelian Randomization Study

IF 2.1 Q2 MEDICINE, GENERAL & INTERNAL Health Science Reports Pub Date : 2024-10-24 DOI:10.1002/hsr2.70162
Kefu Tang, Wenqiu Wang, Weiteng Chang, Xi Wu
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Abstract

Background and Aims

Observational studies suggest that antidiabetic drugs may lower POAG risk; while the causal relationship remains unclear. Naturally occurring variation in genes encoding antidiabetics drug targets can be used as proxies to investigate long-term therapeutic effect of these drugs on POAG risk.

Methods

We performed a two-sample Mendelian randomization study to evaluate the potential effect of antidiabetic drug targets on POAG in Europeans and East Asians. To proxy antidiabetic drugs (ABCC8, PPARG, GLP1R, SLC5A2), we leveraged genetic variants located near or within drug target genes that were associated with HbA1c. The validity of our ancestry-specific genetic instrument was checked with multipul positive control outcomes. Genetic summary statistics of POAG from the International Glaucoma Genetics Consortium, Global Biobank Meta-analysis Initiative, and FinnGen consortia were analyzed for Europeans (38,164 cases and 1,576,179 controls) and East Asians (16,650 cases and 288,833 controls) separately. Inverse-variance weighted random-effects models were used as primary method.

Results

MR results provided consistent evidence of a protective effect of ABCC8 inhibition on POAG using data sets from IGG, GBMI, and FinnGen. Genetically predicted one-standard deviation reduction in HbA1c from ABCC8 inhibition were significant associated with lower risk of POAG in Europeans (OR = 0.211, 95% CI: 0.133–0.333; p < 0.001) and East Asians (OR = 0.070, 95% CI: 0.011–0.459; p = 0.0056). The association between genetically predicted ABCC8 inhibition and risk of POAG was mainly mediated through intraocular pressure. No association was found for PPARG, SLC5A2, or GLP1R. Sensitivity analyses supported this observation.

Conclusions

We found a protective effect of genetically proxied ABCC8 inhibition on POAG risk in both Europeans and East Asians, highlighting ABCC8 as a promising candidate drug target for POAG, and mechanisms underlying the protective effect should also be investigated.

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基因替代抗糖尿病药物靶点与原发性开角型青光眼:孟德尔随机化研究。
背景和目的:观察性研究表明,抗糖尿病药物可降低POAG风险,但其中的因果关系仍不清楚。编码抗糖尿病药物靶点基因的自然发生变异可作为代用品,用于研究这些药物对 POAG 风险的长期治疗效果:我们进行了一项双样本孟德尔随机研究,以评估抗糖尿病药物靶点对欧洲人和东亚人POAG的潜在影响。为了代理抗糖尿病药物(ABCC8、PPARG、GLP1R、SLC5A2),我们利用了位于与 HbA1c 相关的药物靶基因附近或内部的遗传变异。我们的祖先特异性遗传工具的有效性通过多重阳性对照结果进行了检验。我们分别对欧洲人(38164 例病例和 1576179 例对照)和东亚人(16650 例病例和 288833 例对照)进行了分析。主要方法是使用逆方差加权随机效应模型:MR结果利用IGG、GBMI和FinnGen的数据集提供了一致的证据,证明ABCC8抑制剂对POAG具有保护作用。 根据基因预测,ABCC8抑制剂可使HbA1c降低一个标准差,这与欧洲人罹患POAG的风险降低显著相关(OR = 0.211,95% CI:0.133-0.333;P = 0.0056)。基因预测的 ABCC8 抑制与 POAG 风险之间的关联主要是通过眼压介导的。没有发现 PPARG、SLC5A2 或 GLP1R 与此相关。敏感性分析支持这一观点:结论:我们发现,在欧洲人和东亚人中,ABCC8抑制基因对POAG风险具有保护作用。
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来源期刊
Health Science Reports
Health Science Reports Medicine-Medicine (all)
CiteScore
1.80
自引率
0.00%
发文量
458
审稿时长
20 weeks
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