首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Intracoronary shear-related up-regulation of platelet P-selectin and platelet-monocyte aggregation despite the use of aspirin and clopidogrel.
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Intracoronary shear-related up-regulation of platelet P-selectin and platelet-monocyte aggregation despite the use of aspirin and clopidogrel.

机译:尽管使用了阿司匹林和氯吡格雷,但冠状动脉内剪切相关的血小板P选择素和血小板单核细胞聚集的上调。

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摘要

Recent in vitro studies have shown that shear stress can cause platelet activation by agonist-independent pathways. However, no studies have assessed the extent of shear-induced platelet activation within human coronary arteries. We sampled blood from the coronary arteries proximal and distal to coronary lesions and from the coronary sinus in humans with stable coronary disease who were taking both aspirin and clopidogrel. A novel, computationally based technique for estimating shear stress from 3-dimensional coronary angiographic images of these arteries was developed, and the effect of stenosis severity and calculated shear stress on in vivo platelet and related leukocyte activation pathways were determined. We provide evidence of intracoronary up-regulation of platelet P-selectin, platelet-monocyte aggregation, and monocyte CD11b without platelet glycoprotein IIb-IIIa activation or soluble P-selectin up-regulation. This correlates with intracoronary stenosis severity and calculated shear stress and occurs despite the concurrent use of aspirin and clopidogrel. Our results show for the first time shear-related platelet and monocyte activation in human coronary arteries and suggest this as a potential therapeutic target that is resistant to conventional antiplatelet agents.
机译:最近的体外研究表明,剪切应力可以通过非激动剂依赖性途径引起血小板活化。但是,尚无研究评估人冠状动脉内剪切诱导的血小板活化程度。我们从同时服用阿司匹林和氯吡格雷的稳定型冠心病患者的冠状动脉近端和远端冠状动脉以及冠状窦中抽取血液。开发了一种基于计算的新颖技术,可从这些动脉的3维冠状动脉血管造影图像估算切应力,并确定狭窄程度和计算切应力对体内血小板及相关白细胞激活途径的影响。我们提供了冠状动脉内血小板P-选择素,血小板单核细胞聚集和单核细胞CD11b的上调而无血小板糖蛋白IIb-IIIa激活或可溶性P-选择素上调的证据。这与冠状动脉内狭窄的严重程度和计算出的剪切应力有关,尽管同时使用阿司匹林和氯吡格雷仍会发生。我们的结果首次显示了人冠状动脉中与剪切有关的血小板和单核细胞活化,并表明这是对常规抗血小板药具有抗性的潜在治疗靶标。

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