Critical role for platelet Ral GTPases in regulating venous thrombosis in mice.

IF 5.5 2区 医学 Q1 HEMATOLOGY
Yong Li, Jonathan A Furniss, Jordan Vautrinot, Christopher M Williams, Tony G Walsh, Alexander Brill, Borko Amulic, Alastair W Poole
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引用次数: 0

Abstract

Background: Deep vein thrombosis (DVT) is a major cause of morbidity and mortality globally. While its pathophysiology is complex, increasing evidence suggests a more prominent role for platelets than previously suspected. Genetic deletion of Ral GTPases, RalA and RalB, conditionally in mouse platelets (RalAB DKO), results in a near complete defect in P-selectin externalisation upon activation, while other platelet activation responses and arterial thrombosis are preserved.

Objective: Given the critical role of P-selectin in mediating platelet-neutrophil interaction and thromboinflammation, we sought to investigate whether platelet Rals would also play critical roles in venous thrombosis, a thromboinflammatory disease, using RalAB DKO mice.

Methods: DVT was induced by surgical partial ligation of the caudal (inferior) vena cava for 24-h or 48-h before venous thrombi were assessed by histology and immunofluorescence microscopy.

Results: RalAB DKO mice show a reduction in venous thrombus formation after 24-h, and near complete ablation of venous thrombosis by 48-h post IVC ligation. Immunofluorescence microscopy revealed that cross sections of thrombi from wildtype mice consist of an organised scaffolded structure of platelets surrounding leukocytes/neutrophils producing NETs to stabilize and propagate the thrombus. This organised structure was absent in platelet-specific conditional RalAB DKO thrombi. In vitro analysis of platelet-mediated NET formation was also significantly reduced when platelets lacked RalAB or when platelets were treated with the Ral inhibitor RBC8.

Conclusion: We identify platelet Rals as novel, potentially critical regulators of venous thrombus stability, through their ability to regulate neutrophil NET formation via platelet P-selectin.

血小板 Ral GTP 酶在调节小鼠静脉血栓形成中的关键作用。
背景:深静脉血栓(DVT)是全球发病和死亡的主要原因。虽然其病理生理学十分复杂,但越来越多的证据表明,血小板在其中所起的作用比以前所怀疑的更为突出。有条件地在小鼠血小板中基因缺失 Ral GTP 酶 RalA 和 RalB(RalAB DKO)会导致血小板活化时 P 选择素外化几乎完全缺失,而其他血小板活化反应和动脉血栓形成则得以保留:鉴于 P-选择素在介导血小板-中性粒细胞相互作用和血栓性炎症中的关键作用,我们试图利用 RalAB DKO 小鼠研究血小板 Rals 是否也会在静脉血栓形成(一种血栓性炎症疾病)中发挥关键作用:方法:通过手术部分结扎尾(下)腔静脉24小时或48小时诱发深静脉血栓,然后用组织学和免疫荧光显微镜评估静脉血栓:结果:RalAB DKO 小鼠在 24 小时后静脉血栓形成减少,在 IVC 结扎后 48 小时静脉血栓几乎完全消除。免疫荧光显微镜显示,野生型小鼠血栓的横截面由血小板组成的有组织支架结构围绕着产生 NETs 的白细胞/中性粒细胞,以稳定和传播血栓。这种有组织结构在血小板特异性条件性 RalAB DKO 血栓中不存在。体外分析发现,当血小板缺乏 RalAB 或用 Ral 抑制剂 RBC8 处理血小板时,血小板介导的 NET 形成也明显减少:通过血小板 P 选择素调节中性粒细胞 NET 形成的能力,我们发现血小板 Rals 是静脉血栓稳定性的新型潜在关键调节因子。
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来源期刊
Journal of Thrombosis and Haemostasis
Journal of Thrombosis and Haemostasis 医学-外周血管病
CiteScore
24.30
自引率
3.80%
发文量
321
审稿时长
1 months
期刊介绍: The Journal of Thrombosis and Haemostasis (JTH) serves as the official journal of the International Society on Thrombosis and Haemostasis. It is dedicated to advancing science related to thrombosis, bleeding disorders, and vascular biology through the dissemination and exchange of information and ideas within the global research community. Types of Publications: The journal publishes a variety of content, including: Original research reports State-of-the-art reviews Brief reports Case reports Invited commentaries on publications in the Journal Forum articles Correspondence Announcements Scope of Contributions: Editors invite contributions from both fundamental and clinical domains. These include: Basic manuscripts on blood coagulation and fibrinolysis Studies on proteins and reactions related to thrombosis and haemostasis Research on blood platelets and their interactions with other biological systems, such as the vessel wall, blood cells, and invading organisms Clinical manuscripts covering various topics including venous thrombosis, arterial disease, hemophilia, bleeding disorders, and platelet diseases Clinical manuscripts may encompass etiology, diagnostics, prognosis, prevention, and treatment strategies.
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