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冠状动脉狭窄体外模型中的血小板黏附/聚集

Platelet adhesion/aggregation in an in vitro model of coronary artery stenosis.

作者信息

Grabowski E F, Rodriguez M, McDonnell S L

机构信息

Department of Pediatrics, New York Hospital-Cornell Medical Center, New York.

出版信息

Cathet Cardiovasc Diagn. 1993 Jan;28(1):65-71. doi: 10.1002/ccd.1810280113.

DOI:10.1002/ccd.1810280113
PMID:8416335
Abstract

Platelet adhesion/aggregation (PAA) at a site of coronary artery stenosis is believed to be a process strongly modulated by local shear rates and the functional state of neighboring endothelium. One purpose of the present work, therefore, is to describe an in vitro model for the direct imaging of such PAA. Another is to apply the model to the question as to whether the use of nonionic vs. ionic contrast media (CM) in the presence of vascular endothelium contributes to PAA at the stenosis site. Toward these ends, we utilized a special flow chamber which incorporates a monolayer of endothelial cells (ECs), a step 66% flowpath constriction at a site preadsorbed with microfibrillar collagen, and arterial shear rates. By epifluorescence microscopy and digital image analysis of video recordings, PAA was found to be greater with dysfunctional ECs (pretreated with lysine acetylsalicyclate) than with normal ECs, thereby confirming a modulatory role in PAA of functionally intact ECs. When nonionic (iohexol) or ionic (ioxaglate, diatrizoate) CM was added to the flowing blood at a concentration of 20% by non-red cell volume, PAA was inhibited in the order diatrizoate > ioxaglate > iohexol > saline control. No inhibition by any CM was seen, however, when chamber prefill culture medium containing 20% by volume CM was displaced by CM-free blood, in simulation of bolus administration of CM. In terms of inhibition of PAA during percutaneous transluminal coronary angioplasty (PTCA), therefore, our model provides a conceptual basis by which one may anticipate in flowing blood no clear benefit of ionic over nonionic CM.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

冠状动脉狭窄部位的血小板黏附/聚集(PAA)被认为是一个受局部剪切速率和邻近内皮功能状态强烈调节的过程。因此,本研究的一个目的是描述一种用于直接成像此类PAA的体外模型。另一个目的是将该模型应用于以下问题:在血管内皮存在的情况下,使用非离子型与离子型造影剂(CM)是否会导致狭窄部位的PAA。为了实现这些目标,我们使用了一个特殊的流动腔室,该腔室包含单层内皮细胞(ECs)、在预吸附微纤维胶原的部位有66%的流路狭窄以及动脉剪切速率。通过落射荧光显微镜和视频记录的数字图像分析,发现功能失调的ECs(用赖氨酸乙酰水杨酸预处理)比正常ECs的PAA更大,从而证实了功能完整的ECs在PAA中的调节作用。当以非红细胞体积的20%浓度将非离子型(碘海醇)或离子型(碘克沙醇、泛影葡胺)CM添加到流动血液中时,PAA受到抑制,顺序为泛影葡胺>碘克沙醇>碘海醇>生理盐水对照。然而,当用无CM的血液替代含有20%体积CM的腔室预充培养基以模拟CM的团注给药时,未观察到任何CM的抑制作用。因此,就经皮冠状动脉腔内血管成形术(PTCA)期间对PAA的抑制而言,我们的模型提供了一个概念基础,据此人们可以预期在流动血液中离子型CM相对于非离子型CM没有明显益处。(摘要截短于250字)

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Platelet adhesion/aggregation in an in vitro model of coronary artery stenosis.冠状动脉狭窄体外模型中的血小板黏附/聚集
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