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新冠病毒刺突蛋白与血小板激活因子之间是否存在相互作用?

Is there an interplay between the SARS-CoV-2 spike protein and Platelet-Activating factor?

机构信息

Laboratory of Biology, Biochemistry and Microbiology, Department of Nutrition-Dietetics, School of Health Sciences and Education, Harokopio University, Athens, Greece.

Laboratory of Molecular Immunopharmacology and Drug Discovery, Department of Immunology, Tufts University School of Medicine, Boston, Massachusetts, United States.

出版信息

Biofactors. 2022 Nov;48(6):1271-1283. doi: 10.1002/biof.1877. Epub 2022 Jul 19.

Abstract

Previous publications have reported a potent effect of COVID-19 on platelet function and that the Spike protein enhances washed human platelet aggregation induced by various agonists. This study aims to evaluate whether mRNA vaccination for COVID-19 affects human platelet-rich plasma (hPRP) aggregation response, whether a recombinant Spike protein modulates PAF-induced aggregation in hPRP and in washed rabbit platelets (WRP), and to investigate the effect of recombinant Spike protein on the PAF production in the U-937 cell line. Our results showed that PRP from vaccinated individuals exhibited ex vivo lower EC values in response to PAF, ADP, and collagen. Platelet incubation with the Spike protein alone did not induce aggregation either in hPRP or in WRP, but resulted in augmentation of in vitro PAF-induced aggregation in hPRP from non-vaccinated individuals and in WRP. When PRP from vaccinated individuals was incubated with the Spike protein and PAF was subsequently added, elimination of the secondary wave of the biphasic aggregation curve was recorded compared with the aggregation induced by PAF alone. Collagen-induced in vitro aggregation was dose-dependently reduced when platelets were pre-incubated with the Spike protein in all tested aggregation experiments. Stimulation of U-937 by the Spike protein induced an increase in intracellular PAF production accompanied by elevation of the activities of all three PAF biosynthetic enzymes. In conclusion, since the Spike protein appears to modulate PAF production and activity, the use of compounds that act as PAF inhibitors, could be considered at least in mild cases of patients infected with SARS-CoV-2.

摘要

先前的出版物已经报道了 COVID-19 对血小板功能的强大影响,并且 Spike 蛋白增强了各种激动剂诱导的洗涤人类血小板聚集。本研究旨在评估 COVID-19 的 mRNA 疫苗接种是否会影响富含血小板的人血浆 (hPRP) 聚集反应,重组 Spike 蛋白是否调节 hPRP 和洗涤兔血小板 (WRP) 中 PAF 诱导的聚集,以及研究重组 Spike 蛋白对 U-937 细胞系中 PAF 产生的影响。我们的结果表明,接种个体的 PRP 对 PAF、ADP 和胶原的反应表现出较低的 EC 值。Spike 蛋白单独孵育不会引起 hPRP 或 WRP 中的聚集,但会导致非接种个体的 hPRP 和 WRP 中体外 PAF 诱导的聚集增强。当接种个体的 PRP 与 Spike 蛋白孵育,随后加入 PAF 时,与单独用 PAF 诱导的聚集相比,记录到双相聚集曲线的第二波消除。在所有测试的聚集实验中,当血小板在预孵育中用 Spike 蛋白时,胶原诱导的体外聚集呈剂量依赖性降低。Spike 蛋白刺激 U-937 诱导细胞内 PAF 产生增加,同时三种 PAF 生物合成酶的活性升高。总之,由于 Spike 蛋白似乎调节 PAF 的产生和活性,因此可以考虑在感染 SARS-CoV-2 的轻度患者中使用作为 PAF 抑制剂的化合物。

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