Identifying Novel Inflammatory Protein Biomarkers and Drug Targets of Inflammatory Bowel Disease by Integrating Mendelian Randomization, Bioinformatics, and Druggability Analysis.

IF 2.5 4区医学 Q3 ALLERGY

International Archives of Allergy and Immunology Pub Date : 2025-01-17 DOI:10.1159/000543259

Feifan Wang, Lu Chen, Yu Tian

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引用次数: 0

Abstract

Introduction: Inflammatory proteins have the potential to be used as therapeutic targets for inflammatory bowel disease (IBD).

Methods: We conducted Mendelian randomization (MR) analysis to probe causal associations between 91 circulating inflammatory proteins and IBD in the discovery and replication cohorts. Subsequently, we conducted meta-analysis of results from two cohorts. We further conducted protein-protein interaction (PPI), enrichment analysis, and druggability evaluation to elucidate our results and prioritize potential therapeutic targets.

Results: By integrating data from two cohorts, we demonstrated that genetically predicted CD40 (odds ratio (OR) = 0.878, 95% confidence interval (CI) = 0.838-0.919) and C-X-C motif chemokine ligand (CXCL)5 (OR = 0.884, 95% CI = 0.841-0.930) decreased IBD risk. However, genetically predicted CXCL9 (OR = 1.184, 95% CI = 1.084-1.294), interleukin (IL)-18 (OR = 1.140, 95% CI = 1.076-1.208), CD6 (OR = 1.096, 95% CI = 1.045-1.150), and 4E-binding protein 1 (4E-BP1) (OR = 1.154, 95% CI = 1.070-1.244) increased IBD risk. Moreover, genetically predicted CD40 (OR = 0.855, 95% CI = 0.801-0.912) decreased Crohn's disease (CD) risk. Genetically predicted fibroblast growth factor 21 (FGF21) (OR = 1.259, 95% CI = 1.135-1.397) and 4E-BP1 (OR = 1.202, 95% CI = 1.088-1.327) increased CD risk. We found no inflammatory protein associated with ulcerative colitis. Additionally, CD was significantly associated with elevated levels of three circulating inflammatory proteins, which are suggested to be the consequences of CD. PPI analysis demonstrated interactions between CXCL5, CXCL9, IL-18, CD40, and FGF21. Enrichment analysis indicated these identified proteins significantly enriched in inflammation-related signaling pathways, including interleukin signaling, cytokine signaling, and NF-κB pathway. Three proteins (CD40, IL-18, 4E-BP1) have been targeted for drug development on cancers and immune-related diseases, with potentials of therapeutic targets for IBD.

Conclusion: Our results provide new biomarkers and drug targets for CD. Moreover, we further demonstrate critical roles of inflammation and immunity in the occurrence and development of IBD.

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通过整合孟德尔随机化、生物信息学和药物分析，鉴定炎症性肠病的新型炎症蛋白生物标志物和药物靶点。

炎症蛋白有潜力被用作炎症性肠病（IBD）的治疗靶点。方法：我们通过孟德尔随机化（MR）分析，在发现和复制队列中探讨91种循环炎症蛋白与IBD之间的因果关系。随后，我们对两个队列的结果进行了荟萃分析。我们进一步进行了蛋白相互作用（PPI）、富集分析和药物性评估来阐明我们的结果并优先考虑潜在的治疗靶点。结果：通过整合来自两个队列的数据，我们证明基因预测CD40（优势比[OR] = 0.878, 95%可信区间[CI] = 0.838-0.919）和C-X-C基序趋化因子配体（CXCL）5 （OR = 0.884, 95%CI = 0.841-0.930）降低IBD风险。然而，基因预测的CXCL9 （OR = 1.184, 95%CI = 1.084-1.294）、白细胞介素(IL)-18 （OR = 1.140, 95%CI = 1.076-1.208）、CD6 （OR = 1.096, 95%CI = 1.045-1.150）和4e结合蛋白1 (4E-BP1) （OR = 1.154, 95%CI = 1.070-1.244）增加了IBD的风险。此外，基因预测的CD40 （OR = 0.855, 95%CI = 0.801-0.912）降低了克罗恩病（CD）的风险。基因预测成纤维细胞生长因子21 (FGF21) （OR = 1.259, 95%CI = 1.135-1.397）和4E-BP1 （OR = 1.202, 95%CI = 1.088-1.327）增加CD风险。我们没有发现与溃疡性结肠炎相关的炎症蛋白。此外，CD与三种循环炎症蛋白水平升高显著相关，这被认为是CD的后果。PPI分析证实了CXCL5、CXCL9、IL-18、CD40和FGF21之间的相互作用。富集分析表明，这些鉴定的蛋白在炎症相关信号通路中显著富集，包括白细胞介素信号通路、细胞因子信号通路和NF-κB信号通路。三种蛋白（CD40, IL-18, 4E-BP1）已经成为癌症和免疫相关疾病的药物开发靶点，具有治疗IBD的潜力。结论：我们的研究结果为CD提供了新的生物标志物和药物靶点。此外，我们进一步证明了炎症和免疫在IBD发生和发展中的关键作用。

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来源期刊

International Archives of Allergy and Immunology 医学-过敏

CiteScore

5.60

自引率

3.60%

发文量

105

审稿时长

2 months

期刊介绍： ''International Archives of Allergy and Immunology'' provides a forum for basic and clinical research in modern molecular and cellular allergology and immunology. Appearing monthly, the journal publishes original work in the fields of allergy, immunopathology, immunogenetics, immunopharmacology, immunoendocrinology, tumor immunology, mucosal immunity, transplantation and immunology of infectious and connective tissue diseases.