血红素诱导的血小板活化受 ACKR3 趋化因子表面受体的调控,对脆弱的动脉粥样硬化斑块的钝化有影响。

Zoi Laspa, Valerie Dicenta-Baunach, David Schaale, Manuel Sigle, Ravi Hochuli, Tatsiana Castor, Alp Bayrak, Tobias Harm, Karin Anne Lydia Müller, Thanigaimalai Pillaiyar, Stefan Laufer, Anne-Katrin Rohlfing, Meinrad Paul Gawaz
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引用次数: 0

摘要

在易损的动脉粥样硬化斑块中,斑块内出血(IPH)会导致红细胞溶血,释放血红蛋白和游离血红素。血红蛋白激活血小板,导致血栓形成。抑制性血小板受体 ACKR3 的激动作用可抑制血红素依赖性血小板活化和血栓形成。为了描述血红素和 ACKR3 激动对分离的人体血小板的影响,我们使用了多色流式细胞仪和经典的实验装置,如透光聚集测定法和流动室测定法。在 500 s-1 的低剪切速率下,血红素可诱导血小板聚集,并在固定胶原上形成血小板依赖性血栓,这表明游离血红素是血小板依赖性血栓形成的强激活剂。最近,我们发现 ACKR3 是血小板活化的一个重要抑制受体。特异性 ACKR3 激动剂而非传统的抗血小板化合物(如 COX-1 抑制剂(吲哚美辛)、ADP 受体阻断剂(坎格雷洛)或 PAR1 抑制剂(ML161))可抑制血红素依赖性聚集和血栓形成。为了进一步确定血红素对血小板亚群的影响,我们建立了一种多色流式细胞术检测方法。我们发现血凝素能诱导促凝(CD42bpos/PAC-1neg/AnnexinVpos)、聚集(CD42bpos/PAC-1pos/AnnexinVneg)和炎症(CD42bpos/CXCR4pos/ACKR3pos/AnnexinVpos)血小板亚群。用 ACKR3 激动剂治疗可明显减少促凝血血小板和 ACKR3pos 血小板对血氨的反应。我们的结论是,血凝素是一种强激活剂,可促进促凝血小板的形成和血栓的形成,而这取决于 ACKR3 的功能。使用特异性激动剂激活 ACKR3 可为调节 IPH 地区动脉粥样硬化斑块的脆弱性提供一种治疗策略。
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Hemin-induced platelet activation is regulated by the ACKR3 chemokine surface receptor and has implications for passivation of vulnerable atherosclerotic plaques.

In vulnerable atherosclerotic plaques, intraplaque hemorrhages (IPH) result in hemolysis of red blood cells and release of hemoglobin and free hemin. Hemin activates platelets and leads to thrombosis. Agonism of the inhibitory platelet receptor ACKR3 inhibits hemin-dependent platelet activation and thrombus formation. To characterize the effect of hemin and ACKR3 agonism on isolated human platelets, multi-color flow cytometry and classical experimental setup such as light transmission aggregometry and a flow chamber assay were used. Hemin induces platelet aggregation and ex vivo platelet-dependent thrombus formation on immobilized collagen under a low shear rate of 500 s-1, indicating that free hemin is a strong activator of platelet-dependent thrombosis. Recently, we described that ACKR3 is a prominent inhibitory receptor of platelet activation. Specific ACKR3 agonists but not conventional antiplatelet compounds such as COX-1 inhibitor (indometacin), ADP-receptor blocker (cangrelor), or PAR1 inhibitor (ML161) inhibit both hemin-dependent aggregation and thrombus formation. To further characterize the effect of hemin on platelet subpopulations, we established a multi-color flow cytometry assay. We found that hemin induces procoagulant (CD42bpos/PAC-1neg/AnnexinVpos), aggregatory (CD42bpos/PAC-1pos/AnnexinVneg), and inflammatory (CD42bpos/CXCR4pos/ACKR3pos/AnnexinVpos) platelet subpopulations. Treatment with ACKR3 agonists significantly decreased the formation of procoagulant and ACKR3pos platelets in response to hemin. We conclude that hemin is a strong activator for the formation of procoagulant platelets and thrombus formation which is dependent on the function of ACKR3. Activation of ACKR3 using specific agonists may offer a therapeutic strategy to regulate the vulnerability of atherosclerotic plaques in areas of IPH.

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