[Optimization and identification of potential targets of obacunone against sepsis].

Q3 Medicine

Zhonghua wei zhong bing ji jiu yi xue Pub Date : 2024-08-01 DOI:10.3760/cma.j.cn121430-20231129-01019

Yuting Chen, Yunong Liu, Chang Liu, Yubin Xu, Guirong Chen

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引用次数: 0

Abstract

Objective: To investigate the molecular characteristics of obacunone, and to screen and identify potential targets of obacunone against sepsis.

Methods: The pharmacological parameters and molecular characteristics of obacunone were analyzed with the aid of the Traditional Chinese Medicine Systems Pharmacology Database Analysis Platform (TCMSP). The potential targets of obacunone against sepsis were screened using SwissTargetPrediction and Drug Repositioning and Adverse Drug Reaction Chemical-Protein Interactome (DRAR-CPI) software, with a Z'-score < -0.5. The anti-sepsis targets of obacunone were selected by Online Mendelian Inheritance in Man (OMIM), Comparative Toxicogenomics Database (CTD) and Therapeutic Target Database (TTD). The anti-sepsis potential target was identified by molecular docking software.

Results: The oral bioavailability of obacunone was 81.58% and the drug-likeness was 0.57 indicating that obacunone showed good drug formation. A total of 242 potential targets were screened through SwissTargetPrediction and DRAR-CPI software, 13 targets were directly related to sepsis. Cathepsin G (CTSG), caspase-1 (CASP1), S100 calcium binding protein A9 (S100A9), protein C (inactivator of coagulation factors V a and VIII a, PROC), mitogen-activated protein kinase 1 (MAPK1), glucose-6-phosphate dehydrogenase (G6PD), interleukin-10 (IL-10), migration inhibitory factor (MIF), complement C5a receptor 1 (C5AR1), caspase-3 (CASP3), CXC chemokine receptor 2 (CXCR2), thrombin receptor (F2R), nicotinamide phosphoribosyltransferase (NAMPT) were identified as the potential targets for anti-sepsis of obacunone by molecular docking software, the free binding energies were -32.55, 1.26, -30.00, 300.08, -31.88, -30.29, -21.38, -30.79, 16 777.84, -21.80, 6 443.36, -20.38, -23.47 kJ/mol, respectively.

Conclusions: Obacunone can inhibit blood coagulation and improve inflammatory response by regulating PROC and F2R. It regulates MIF, S100A9, G6PD and IL-10 to play a role in immune response. It regulates CTSG, CASP1, MAPK1, C5AR1 and CASP3 to protect sepsis-damaged organs. By regulating CXCR2, it can reduce the excessive migration of neutrophils to the site of inflammation, alleviate tissue damage. By regulating NAMPT, it improves cellular energy status, reduces oxidative stress, and protects cells from damage.

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[优化和确定乌巴骨醌抗败血症的潜在靶点]。

目的方法：借助中药系统药理学数据库分析平台（TCMSP），分析欧巴酮的药理参数和分子特征：方法：借助中药系统药理数据库分析平台（TCMSP）分析了乌药酮的药理参数和分子特征。利用SwissTargetPrediction和Drug Repositioning and Adverse Drug Reaction Chemical-Protein Interactome (DRAR-CPI)软件筛选出顺铂酮抗脓毒症的潜在靶点，Z'-score<-0.5。通过在线人类孟德尔遗传（OMIM）、比较毒物基因组学数据库（CTD）和治疗靶点数据库（TTD）筛选出了欧巴酮的抗败血症靶点。通过分子对接软件确定了抗败血症的潜在靶点：结果：欧巴铜酮的口服生物利用度为 81.58%，药物相似度为 0.57，表明欧巴铜酮具有良好的成药性。通过SwissTargetPrediction和DRAR-CPI软件共筛选出242个潜在靶点，其中13个靶点与败血症直接相关。这些靶标包括：凝血酶 G（CTSG）、Caspase-1（CASP1）、S100钙结合蛋白 A9（S100A9）、蛋白 C（凝血因子 V a 和 VIII a 的灭活剂，PROC）、丝裂原活化蛋白激酶 1（MAPK1）、葡萄糖-6-磷酸脱氢酶（G6PD）、白细胞介素-10（IL-10）、迁移抑制因子（MIF）、通过分子对接软件，确定了补体 C5a 受体 1（C5AR1）、Caspase-3（CASP3）、CXC 趋化因子受体 2（CXCR2）、凝血酶受体（F2R）、烟酰胺磷酸核糖转移酶（NAMPT）为欧巴铜酮抗败血症的潜在靶点，其自由结合能分别为-32.55、1.26、-30.00、300.08、-31.88、-30.29、-21.38、-30.79、16 777.84、-21.80、6 443.36、-20.38、-23.47 kJ/mol.结论：奥巴昆酮可通过调节 PROC 和 F2R 抑制血液凝固，改善炎症反应。奥巴昆酮能调节 MIF、S100A9、G6PD 和 IL-10，在免疫反应中发挥作用。它能调节 CTSG、CASP1、MAPK1、C5AR1 和 CASP3，保护败血症受损器官。通过调节 CXCR2，它可以减少中性粒细胞向炎症部位的过度迁移，减轻组织损伤。通过调节 NAMPT，它能改善细胞能量状态，减少氧化应激，保护细胞免受损伤。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Zhonghua wei zhong bing ji jiu yi xue Medicine-Critical Care and Intensive Care Medicine

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1.00

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0.00%

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