Yingjie Bai, Jiayi Wang, Xuefeng Feng, Le Xie, Shengao Qin, Guowu Ma, Fan Zhang
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Moreover, to delve deeper into potential regulation among DNA methylation, gene expression, and protein abundance, we conducted MR analysis to explore the causal relationship between candidate gene methylation and expression, as well as between gene expression and protein abundance. Drug prediction and molecular docking were further employed to validate the pharmacological activity of the candidate drug targets.Upon integrating the multi-omics data, we identified three genes associated with SS risk: TNFAIP3, BTN3A1, and PLAU. The methylation of cg22068371 in BTN3A1 was positively associated with protein levels, consistent with the negative effect of cg22068371 methylation on the risk of SS. Additionally, positive correlations were observed between the gene methylation of PLAU (cg04939496) and expression, as well as between expression and protein levels. This consistency elucidates the promotional effects of PLAU on SS risk at the DNA methylation, gene expression, and protein levels. At the protein level, genetically predicted TNFAIP3 (OR 2.47, 95% CI 1.56–3.92) was positively associated with SS risk, while BTN3A1 (OR 2.96E-03, 95% CI 2.63E-04–3.33E-02) was negatively associated with SS risk. Molecular docking showed stable binding for candidate drugs and target proteins.Our study reveals promising therapeutic targets for the treatment of SS, providing valuable insights into targeted therapy for SS. However, further validation through future experiments is warranted.","PeriodicalId":505785,"journal":{"name":"Frontiers in Immunology","volume":"40 10","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2024-06-12","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Identification of drug targets for Sjögren’s syndrome: multi-omics Mendelian randomization and colocalization analyses\",\"authors\":\"Yingjie Bai, Jiayi Wang, Xuefeng Feng, Le Xie, Shengao Qin, Guowu Ma, Fan Zhang\",\"doi\":\"10.3389/fimmu.2024.1419363\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"Targeted therapy for Sjögren’s syndrome (SS) has become an important focus for clinicians. Multi-omics-wide Mendelian randomization (MR) analyses have provided new ideas for identifying potential drug targets.We conducted summary-data-based Mendelian randomization (SMR) analysis to evaluate therapeutic targets associated with SS by integrating DNA methylation, gene expression and protein quantitative trait loci (mQTL, eQTL, and pQTL, respectively). Genetic associations with SS were derived from the FinnGen study (discovery) and the GWAS catalog (replication). Colocalization analyses were employed to determine whether two potentially relevant phenotypes share the same genetic factors in a given region. Moreover, to delve deeper into potential regulation among DNA methylation, gene expression, and protein abundance, we conducted MR analysis to explore the causal relationship between candidate gene methylation and expression, as well as between gene expression and protein abundance. Drug prediction and molecular docking were further employed to validate the pharmacological activity of the candidate drug targets.Upon integrating the multi-omics data, we identified three genes associated with SS risk: TNFAIP3, BTN3A1, and PLAU. The methylation of cg22068371 in BTN3A1 was positively associated with protein levels, consistent with the negative effect of cg22068371 methylation on the risk of SS. Additionally, positive correlations were observed between the gene methylation of PLAU (cg04939496) and expression, as well as between expression and protein levels. This consistency elucidates the promotional effects of PLAU on SS risk at the DNA methylation, gene expression, and protein levels. At the protein level, genetically predicted TNFAIP3 (OR 2.47, 95% CI 1.56–3.92) was positively associated with SS risk, while BTN3A1 (OR 2.96E-03, 95% CI 2.63E-04–3.33E-02) was negatively associated with SS risk. 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引用次数: 0
摘要
针对斯约格伦综合征(SS)的靶向治疗已成为临床医生关注的焦点。我们进行了基于汇总数据的孟德尔随机化(SMR)分析,通过整合 DNA 甲基化、基因表达和蛋白质定量性状位点(分别为 mQTL、eQTL 和 pQTL)来评估与 SS 相关的治疗靶点。与 SS 相关的基因来自 FinnGen 研究(发现)和 GWAS 目录(复制)。共定位分析用于确定两个潜在的相关表型在特定区域是否具有相同的遗传因子。此外,为了深入研究 DNA 甲基化、基因表达和蛋白质丰度之间的潜在调控关系,我们进行了 MR 分析,以探索候选基因甲基化与表达之间以及基因表达与蛋白质丰度之间的因果关系。在整合多组学数据后,我们发现了三个与 SS 风险相关的基因:整合多组学数据后,我们发现了三个与 SS 风险相关的基因:TNFAIP3、BTN3A1 和 PLAU。BTN3A1 中 cg22068371 的甲基化与蛋白水平呈正相关,这与 cg22068371 甲基化对 SS 风险的负面影响一致。此外,还观察到 PLAU(cg04939496)的基因甲基化与表达之间以及表达与蛋白质水平之间存在正相关。这种一致性阐明了 PLAU 在 DNA 甲基化、基因表达和蛋白质水平上对 SS 风险的促进作用。在蛋白质水平上,基因预测的 TNFAIP3(OR 2.47,95% CI 1.56-3.92)与 SS 风险呈正相关,而 BTN3A1(OR 2.96E-03,95% CI 2.63E-04-3.33E-02)与 SS 风险呈负相关。我们的研究揭示了治疗SS的有希望的治疗靶点,为SS的靶向治疗提供了有价值的见解。我们的研究揭示了治疗 SS 的有希望的治疗靶点,为 SS 的靶向治疗提供了有价值的见解,但还需要通过未来的实验进一步验证。
Identification of drug targets for Sjögren’s syndrome: multi-omics Mendelian randomization and colocalization analyses
Targeted therapy for Sjögren’s syndrome (SS) has become an important focus for clinicians. Multi-omics-wide Mendelian randomization (MR) analyses have provided new ideas for identifying potential drug targets.We conducted summary-data-based Mendelian randomization (SMR) analysis to evaluate therapeutic targets associated with SS by integrating DNA methylation, gene expression and protein quantitative trait loci (mQTL, eQTL, and pQTL, respectively). Genetic associations with SS were derived from the FinnGen study (discovery) and the GWAS catalog (replication). Colocalization analyses were employed to determine whether two potentially relevant phenotypes share the same genetic factors in a given region. Moreover, to delve deeper into potential regulation among DNA methylation, gene expression, and protein abundance, we conducted MR analysis to explore the causal relationship between candidate gene methylation and expression, as well as between gene expression and protein abundance. Drug prediction and molecular docking were further employed to validate the pharmacological activity of the candidate drug targets.Upon integrating the multi-omics data, we identified three genes associated with SS risk: TNFAIP3, BTN3A1, and PLAU. The methylation of cg22068371 in BTN3A1 was positively associated with protein levels, consistent with the negative effect of cg22068371 methylation on the risk of SS. Additionally, positive correlations were observed between the gene methylation of PLAU (cg04939496) and expression, as well as between expression and protein levels. This consistency elucidates the promotional effects of PLAU on SS risk at the DNA methylation, gene expression, and protein levels. At the protein level, genetically predicted TNFAIP3 (OR 2.47, 95% CI 1.56–3.92) was positively associated with SS risk, while BTN3A1 (OR 2.96E-03, 95% CI 2.63E-04–3.33E-02) was negatively associated with SS risk. Molecular docking showed stable binding for candidate drugs and target proteins.Our study reveals promising therapeutic targets for the treatment of SS, providing valuable insights into targeted therapy for SS. However, further validation through future experiments is warranted.
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