载脂蛋白A-I在创伤患者中升高,抑制血小板活化并降低凝块强度

IF 2.5 3区 医学 Q3 CELL BIOLOGY Platelets Pub Date : 2022-11-17 Epub Date: 2022-06-05 DOI:10.1080/09537104.2022.2078488
Wilbert L Jones, Christopher R Ramos, Anirban Banerjee, Ernest E Moore, Kirk C Hansen, Julia R Coleman, Marguerite Kelher, Keith B Neeves, Christopher C Silliman, Jorge Di Paola, Brian Branchford
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引用次数: 2

摘要

载脂蛋白a - i (ApoA-I)在全身性高纤溶性创伤患者亚组血浆中升高。我们假设apoA-I抑制血小板活化和凝块形成。通过全血血栓造影(TEG)、血小板聚集、p -选择素表面表达、微流体粘附和Akt磷酸化评估apoA-I对人血小板活化和血栓形成的影响。采用小鼠颈动脉血栓形成和肺栓塞模型评价apoa - 1在体内的作用。采用转基因小鼠敲除(KO)方法研究了清道夫受体B类成员1 (SR-BI)的ApoA-1受体。与对照组相比,外源性人apoA-I抑制花生四烯酸和胶原介导的人和小鼠血小板聚集,降低p -选择素表面表达和Akt活化,导致凝块强度降低,TEG溶解凝块增加。ApoA-I还能降低胶原表面形成的血小板聚集大小。在体内,apoa - 1在动脉血栓形成模型中延迟血管闭塞,在肺栓塞模型中赋予生存优势。与野生型血小板相比,SR-BI KO小鼠显著降低了apoA-I对血小板聚集的抑制作用。外源性人apoA-I通过SR-BI受体抑制血小板活化,降低凝块强度和稳定性,并保护小鼠免受动脉和静脉血栓形成。
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Apolipoprotein A-I, elevated in trauma patients, inhibits platelet activation and decreases clot strength.

Apolipoprotein A-I (ApoA-I) is elevated in the plasma of a subgroup of trauma patients with systemic hyperfibrinolysis. We hypothesize that apoA-I inhibits platelet activation and clot formation. The effects of apoA-I on human platelet activation and clot formation were assessed by whole blood thrombelastography (TEG), platelet aggregometry, P-selectin surface expression, microfluidic adhesion, and Akt phosphorylation. Mouse models of carotid artery thrombosis and pulmonary embolism were used to assess the effects of apoA-I in vivo. The ApoA-1 receptor was investigated with transgenic mice knockouts (KO) for the scavenger receptor class B member 1 (SR-BI). Compared to controls, exogenous human apoA-I inhibited arachidonic acid and collagen-mediated human and mouse platelet aggregation, decreased P-selectin surface expression and Akt activation, resulting in diminished clot strength and increased clot lysis by TEG. ApoA-I also decreased platelet aggregate size formed on a collagen surface under flow. In vivo, apoA-I delayed vessel occlusion in an arterial thrombosis model and conferred a survival advantage in a pulmonary embolism model. SR-BI KO mice significantly reduced apoA-I inhibition of platelet aggregation versus wild-type platelets. Exogenous human apoA-I inhibits platelet activation, decreases clot strength and stability, and protects mice from arterial and venous thrombosis via the SR-BI receptor.

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来源期刊
Platelets
Platelets 医学-细胞生物学
CiteScore
6.70
自引率
3.00%
发文量
79
审稿时长
1 months
期刊介绍: Platelets is an international, peer-reviewed journal covering all aspects of platelet- and megakaryocyte-related research. Platelets provides the opportunity for contributors and readers across scientific disciplines to engage with new information about blood platelets. The journal’s Methods section aims to improve standardization between laboratories and to help researchers replicate difficult methods. Research areas include: Platelet function Biochemistry Signal transduction Pharmacology and therapeutics Interaction with other cells in the blood vessel wall The contribution of platelets and platelet-derived products to health and disease The journal publishes original articles, fast-track articles, review articles, systematic reviews, methods papers, short communications, case reports, opinion articles, commentaries, gene of the issue, and letters to the editor. Platelets operates a single-blind peer review policy. Authors can choose to publish gold open access in this journal.
期刊最新文献
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