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一种来自 的植物前列腺素烷通过潜在结合 EP3 前列腺素受体增加血小板活化、血小板与白细胞的黏附和内皮细胞迁移。

A Phytoprostane from Increases Platelet Activation, Platelet Adhesion to Leukocytes and Endothelial Cell Migration by Potential Binding to EP3 Prostaglandin Receptor.

机构信息

Izpisua Lab, HiTech, Health Sciences Department, Universidad Católica de Murcia (UCAM), Campus de los Jerónimos 135, 30107 Guadalupe, Spain.

Structural Bioinformatics and High-Performance Computing Research Group (BIO-HPC), Computer Engineering Department, Universidad Católica de Murcia (UCAM), Campus de los Jerónimos 135, 30107 Guadalupe, Spain.

出版信息

Int J Mol Sci. 2023 Feb 1;24(3):2730. doi: 10.3390/ijms24032730.

Abstract

Plant phytoprostanes (PhytoPs) are lipid oxidative stress mediators that share structural similarities with mammal prostaglandins (PGs). They have been demonstrated to modulate inflammatory processes mediated by prostaglandins. The present study aims to test the effects of the most abundant oxylipin from , ent-9-D1t-Phytoprostane (9-D1t-PhytoP), on platelet activation and vascular cells as well as clarify possible interactions with platelets and the endothelial EP3 receptor Platelet and monocyte activation was assessed by flow cytometry in the presence of purified 9-D1t-PhytoP. Cell migration was studied using the human Ea.hy926 cell line by performing a scratch wound healing assay. The RNA expression of inflammatory markers was evaluated by RT-PCR under inflammatory conditions. Blind docking consensus was applied to the study of the interactions of selected ligands against the EP3 receptor protein. The 9D1t-PhytoP exerts several pharmacological effects; these include prothrombotic and wound-healing properties. In endothelial cells, 9D1t-PhytP mimics the migration stimulus of PGE. Computational analysis revealed that 9D1t-PhytP forms a stable complex with the hydrophobic pocket of the EP3 receptor by interaction with the same residues as misoprostol and prostaglandin E (PGE), thus supporting its potential as an EP3 agonist. The potential to form procoagulant platelets and the higher endothelial migration rate of the 9-D1t-PhytoP, together with its capability to interact with PGE main target receptor in platelets suggest herein that this oxylipin could be a strong candidate for pharmaceutical research from a multitarget perspective.

摘要

植物类二十烷酸(PhytoPs)是脂质氧化应激介质,与哺乳动物前列腺素(PGs)具有结构相似性。它们已被证明可以调节由前列腺素介导的炎症过程。本研究旨在测试最丰富的氧化脂类物质,ent-9-D1t-Phytoprostane(9-D1t-PhytoP)对血小板激活和血管细胞的影响,并阐明其与血小板和内皮 EP3 受体的可能相互作用。在存在纯化的 9-D1t-PhytoP 的情况下,通过流式细胞术评估血小板和单核细胞的激活。使用划痕愈合测定法,通过人 Ea.hy926 细胞系研究细胞迁移。在炎症条件下,通过 RT-PCR 评估炎症标志物的 RNA 表达。盲法对接共识用于研究针对 EP3 受体蛋白的选定配体的相互作用。9D1t-PhytoP 发挥了几种药理作用;这些作用包括促血栓形成和伤口愈合特性。在内皮细胞中,9D1t-PhytoP 模拟 PGE 的迁移刺激。计算分析表明,9D1t-PhytoP 通过与米索前列醇和前列腺素 E(PGE)相同的残基相互作用,与 EP3 受体的疏水性口袋形成稳定的复合物,从而支持其作为 EP3 激动剂的潜力。形成促凝血小板的潜力和 9-D1t-PhytoP 较高的内皮细胞迁移率,以及其与血小板中 PGE 主要靶受体相互作用的能力表明,这种氧化脂类物质可能是从多靶点角度进行药物研究的强有力候选物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/66a6/9916792/7e2b79fba3a5/ijms-24-02730-g001.jpg

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