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碘海醇、血小板活化与血栓形成。II. 碘海醇诱导的血小板分泌不影响在经肝素和阿司匹林抗凝的血液中由胶原或组织因子诱导的血栓形成。

Iohexol, platelet activation and thrombosis. II. Iohexol-induced platelet secretion does not affect collagen-induced or tissue-factor-induced thrombus formation in blood that is anticoagulated with heparin and aspirin.

作者信息

Sakariassen K S, Buchmann M, Hamers M J, Stormorken H

机构信息

Nycomed Imaging AS, Bioreg Research, Oslo, Norway.

出版信息

Acta Radiol. 1998 Jul;39(4):355-61. doi: 10.1080/02841859809172444.

DOI:10.1080/02841859809172444
PMID:9685818
Abstract

BACKGROUND

There is a dispute about the potential effects of radiographic contrast media (CM) on thrombogenesis. The nonionic CM iohexol triggers platelet beta-thromboglobulin (beta-TG) secretion, and thus may activate the platelets and promote thrombosis. We addressed this topic in a study employing a human model of arterial thrombus formation in the presence of aspirin and heparin. This was a follow-up to our initial study (on thrombus formation in native blood) which did not include antithrombotic drugs. The nonionic CM iohexol (monomer) and iodixanol (dimer) and the ionic CM ioxaglate (dimer) were compared.

METHODS AND RESULTS

Thrombus formation was triggered by a surface rich in either collagen or tissue factor, positioned in a parallel-plate perfusion chamber device at an arterial wall shear rate of 2600 s-1. Blood from healthy volunteers, following ingestion of 1 g aspirin, was mixed with 40 vol% CM and 2.0 IU/ml heparin and passed over the surfaces. Thrombus formation in the presence of either CM showed no difference, despite the fact that iohexol triggered a pronounced platelet beta-TG secretion; iodixanol or ioxaglate were virtually inert.

CONCLUSION

There was no association between iohexol-induced beta-TG secretion and thrombus formation on collagen (platelet-driven) or on tissue factor (thrombin-driven) in the presence of a standard antithrombotic regimen of aspirin and heparin as used in the clinic. The notion of a thrombotic risk due to platelet activation by iohexol was thus not substantiated by this study.

摘要

背景

关于放射造影剂(CM)对血栓形成的潜在影响存在争议。非离子型CM碘海醇可引发血小板β-血小板球蛋白(β-TG)分泌,因此可能激活血小板并促进血栓形成。我们在一项采用阿司匹林和肝素存在下的人体动脉血栓形成模型的研究中探讨了这一话题。这是我们最初研究(关于天然血液中的血栓形成)的后续研究,最初的研究未包括抗血栓药物。对非离子型CM碘海醇(单体)、碘克沙醇(二聚体)和离子型CM碘克酸(二聚体)进行了比较。

方法与结果

血栓形成由富含胶原蛋白或组织因子的表面触发,该表面置于平行板灌注室装置中,动脉壁剪切速率为2600 s-1。健康志愿者服用1 g阿司匹林后的血液与40体积%的CM和2.0 IU/ml肝素混合,然后通过这些表面。尽管碘海醇引发了明显的血小板β-TG分泌,但在任何一种CM存在下的血栓形成均无差异;碘克沙醇或碘克酸几乎无活性。

结论

在临床使用的阿司匹林和肝素标准抗血栓治疗方案存在的情况下,碘海醇诱导的β-TG分泌与胶原蛋白(血小板驱动)或组织因子(凝血酶驱动)上的血栓形成之间没有关联。因此,本研究并未证实碘海醇激活血小板会导致血栓形成风险这一观点。

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