Departamento de Virologia, Instituto de Microbiologia Paulo de Góes, Universidade Federal do Rio de Janeiro, Rio de Janeiro 21941-902, Brazil.
Viruses. 2024 Feb 3;16(2):245. doi: 10.3390/v16020245.
Microcirculatory and coagulation disturbances commonly occur as pathological manifestations of systemic viral infections. Research exploring the role of the kallikrein-kinin system (KKS) in flavivirus infections has recently linked microvascular dysfunctions to bradykinin (BK)-induced signaling of B2R, a G protein-coupled receptor (GPCR) constitutively expressed by endothelial cells. The relevance of KKS activation as an innate response to viral infections has gained increasing attention, particularly after the reports regarding thrombogenic events during COVID-19. BK receptor (B2R and B1R) signal transduction results in vascular permeability, edema formation, angiogenesis, and pain. Recent findings unveiling the role of KKS in viral pathogenesis include evidence of increased activation of KKS with elevated levels of BK and its metabolites in both intravascular and tissue milieu, as well as reports demonstrating that virus replication stimulates BKR expression. In this review, we will discuss the mechanisms triggered by virus replication and by virus-induced inflammatory responses that may stimulate KKS. We also explore how KKS activation and BK signaling may impact virus pathogenesis and further discuss the potential therapeutic application of BKR antagonists in the treatment of hemorrhagic and respiratory diseases.
微循环和凝血障碍通常作为全身病毒感染的病理表现出现。研究探索激肽释放酶-激肽系统(KKS)在黄病毒感染中的作用,将微血管功能障碍与缓激肽(BK)诱导的内皮细胞表达的 G 蛋白偶联受体(B2R)信号联系起来。KKS 激活作为对病毒感染的先天反应的相关性越来越受到关注,特别是在 COVID-19 期间发生血栓形成事件的报道之后。BK 受体(B2R 和 B1R)信号转导导致血管通透性增加、水肿形成、血管生成和疼痛。最近揭示 KKS 在病毒发病机制中的作用的发现包括证据表明,在血管内和组织环境中,KKS 的激活增加,BK 及其代谢物水平升高,以及报告表明病毒复制刺激 BKR 表达。在这篇综述中,我们将讨论病毒复制和病毒诱导的炎症反应触发的机制,这些机制可能会刺激 KKS。我们还探讨了 KKS 激活和 BK 信号如何影响病毒发病机制,并进一步讨论了 BKR 拮抗剂在治疗出血性和呼吸道疾病中的潜在治疗应用。
