Inflammation and thrombosis in COVID-19 pathophysiology: proteinase-activated and purinergic receptors as drivers and candidate therapeutic targets.

IF 29.9 1区 医学 Q1 PHYSIOLOGY Physiological reviews Pub Date : 2021-04-01 Epub Date: 2020-10-30 DOI:10.1152/physrev.00035.2020
Krishna Sriram, Paul A Insel
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引用次数: 73

Abstract

Evolving information has identified disease mechanisms and dysregulation of host biology that might be targeted therapeutically in coronavirus disease 2019 (COVID-19). Thrombosis and coagulopathy, associated with pulmonary injury and inflammation, are emerging clinical features of COVID-19. We present a framework for mechanisms of thrombosis in COVID-19 that initially derive from interaction of SARS-CoV-2 with ACE2, resulting in dysregulation of angiotensin signaling and subsequent inflammation and tissue injury. These responses result in increased signaling by thrombin (proteinase-activated) and purinergic receptors, which promote platelet activation and exert pathological effects on other cell types (e.g., endothelial cells, epithelial cells, and fibroblasts), further enhancing inflammation and injury. Inhibitors of thrombin and purinergic receptors may, thus, have therapeutic effects by blunting platelet-mediated thromboinflammation and dysfunction in other cell types. Such inhibitors include agents (e.g., anti-platelet drugs) approved for other indications, and that could be repurposed to treat, and potentially improve the outcome of, COVID-19 patients. COVID-19, caused by the SARS-CoV-2 virus, drives dysregulation of angiotensin signaling, which, in turn, increases thrombin-mediated and purinergic-mediated activation of platelets and increase in inflammation. This thromboinflammation impacts the lungs and can also have systemic effects. Inhibitors of receptors that drive platelet activation or inhibitors of the coagulation cascade provide opportunities to treat COVID-19 thromboinflammation.

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COVID-19的炎症和血栓病理生理:蛋白酶激活和嘌呤能受体作为驱动因素和候选治疗靶点。
不断发展的信息已经确定了2019冠状病毒病(COVID-19)的疾病机制和宿主生物学失调,这些机制和失调可能是靶向治疗的靶点。与肺损伤和炎症相关的血栓形成和凝血功能障碍是新出现的COVID-19临床特征。我们提出了COVID-19血栓形成机制的框架,该机制最初源于SARS-CoV-2与ACE2的相互作用,导致血管紧张素信号失调,随后出现炎症和组织损伤。这些反应导致凝血酶(蛋白酶激活)和嘌呤能受体信号的增加,从而促进血小板活化并对其他细胞类型(如内皮细胞、上皮细胞和成纤维细胞)产生病理作用,进一步增强炎症和损伤。因此,凝血酶和嘌呤能受体的抑制剂可能通过钝化血小板介导的血栓炎症和其他细胞类型的功能障碍而具有治疗作用。此类抑制剂包括批准用于其他适应症的药物(例如抗血小板药物),这些药物可以重新用于治疗COVID-19患者并可能改善其预后。由SARS-CoV-2病毒引起的COVID-19会导致血管紧张素信号失调,进而增加凝血酶介导和嘌呤能介导的血小板活化,并增加炎症。这种血栓炎症影响肺部,也可能有全身影响。驱动血小板活化的受体抑制剂或凝血级联抑制剂为治疗COVID-19血栓炎症提供了机会。
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来源期刊
Physiological reviews
Physiological reviews 医学-生理学
CiteScore
56.50
自引率
0.90%
发文量
53
期刊介绍: Physiological Reviews is a highly regarded journal that covers timely issues in physiological and biomedical sciences. It is targeted towards physiologists, neuroscientists, cell biologists, biophysicists, and clinicians with a special interest in pathophysiology. The journal has an ISSN of 0031-9333 for print and 1522-1210 for online versions. It has a unique publishing frequency where articles are published individually, but regular quarterly issues are also released in January, April, July, and October. The articles in this journal provide state-of-the-art and comprehensive coverage of various topics. They are valuable for teaching and research purposes as they offer interesting and clearly written updates on important new developments. Physiological Reviews holds a prominent position in the scientific community and consistently ranks as the most impactful journal in the field of physiology.
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