Promising therapeutic targets for ischemic stroke identified from plasma and cerebrospinal fluid proteomes: A multicenter mendelian randomization study

医学 孟德尔随机化 生命银行 生物信息学 内科学 计算生物学 遗传变异 基因型 基因 生物 遗传学
作者
Xuelun Zou,Lei‐Yun Wang,Shun Wang,Yupeng Zhang,Jianyong Ma,Lei Chen,Ye Li,Tian-Xing Yao,Huifang Zhou,Lianxu Wu,Qiaoling Tang,Siyuan Ma,Xiangbin Zhang,Rongmei Tang,Yuting Yi,Yizhi Liu,Yi Zeng,Le Zhang
出处
期刊:International Journal of Surgery [Elsevier]
卷期号:110 (2): 766-776
标识
DOI:10.1097/js9.0000000000000922
摘要

Ischemic stroke (IS) is more common every year, the condition is serious, and have a poor prognosis. New, efficient, and safe therapeutic targets are desperately needed as early treatment especially prevention and reperfusion is the key to lowering the occurrence of poorer prognosis. Generally circulating proteins are attractive therapeutic targets, this study aims to identify potential pharmacological targets among plasma and cerebrospinal fluid (CSF) proteins for the prevention and treatment of IS using a multicenter Mendelian randomization (MR) approach.First, the genetic instruments of 734 plasma and 151 CSF proteins were assessed for causative connections with IS from MEGASTROKE consortium by MR to identify prospective therapeutic targets. Then, for additional validation, plasma proteins from the deCODE consortium and the Fenland consortium, as well as IS GWAS data from the FinnGen cohort, the ISGC consortium and UK biobank, were employed. A thorough evaluation of the aforementioned possible pharmacological targets was carried out using meta-analysis. The robustness of MR results was then confirmed through sensitivity analysis using several techniques, such as bidirectional MR analysis, Steiger filtering, and Bayesian co-localization. Finally, methods like Protein-Protein Interaction (PPI) Networking were utilized to investigate the relationship between putative drug targets and therapeutic agents.We discovered 3 proteins that may function as promising therapeutic targets for IS and meet the Bonferroni correction (P<0.05/885=5.65×10-5). Prekallikrein (OR=0.41, 95%CI: 0.27-0.63, P=3.61×10-5), a protein found in CSF, has a 10-fold protective impact in IS, while the plasma proteins SWAP70 (OR=0.85, 95%CI: 0.80-0.91, P=1.64×10-6) and MMP-12 (OR=0.92, 95%CI: 0.89-0.95, P=4.49×10-6) of each SD play a protective role in IS. Prekallikrein, MMP-12, SWAP70 was replicated in the FinnGen cohort and ISGC database. MMP-12 (OR=0.93, 95%CI: 0.91-0.94, P<0.001), SWAP70 (OR=0.92, 95%CI: 0.90-0.94, P<0.001), and prekallikrein (OR=0.53, 95%CI: 0.33-0.72, P<0.001) may all be viable targets for IS, according to the combined meta-analysis results. Additionally, no evidence of reverse causality was identified, and Bayesian co-localization revealed MMP-12 (PPH4=0.995), SWAP70(PPH4=0.987) and prekallikrein(PPH4=0.894) shared the same variant with IS, supporting the robustness of the aforementioned causation. Prekallikrein and MMP-12 were associated with the target protein of the current treatment of IS. Among them, Lanadelumab, a new drug whose target protein is a prekallikrein, may be a promising new drug for the treatment of IS.The prekallikrein, MMP-12 and SWAP70 are causally associated with the risk of IS. Moreover, MMP-12 and prekallikrein may be treated as promising therapeutic targets for medical intervention of IS.
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