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首页> 外文期刊>Anesthesia and Analgesia: Journal of the International Anesthesia Research Society >Carbon monoxide releasing molecule-2 enhances coagulation and diminishes fibrinolytic vulnerability in plasma exposed to heparin or argatroban.
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Carbon monoxide releasing molecule-2 enhances coagulation and diminishes fibrinolytic vulnerability in plasma exposed to heparin or argatroban.

机译:一氧化碳释放分子2增强了凝血并减少了暴露于肝素或阿加曲班的血浆中的纤溶敏感性。

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摘要

BACKGROUND: It has been recently demonstrated that a carbon monoxide releasing molecule (tricarbonyldichlororuthenium [II] dimer; CORM-2) enhances coagulation and attenuates vulnerability to fibrinolysis in normal and hemophiliac human plasma. We tested the hypothesis that plasma anticoagulated with heparin or argatroban would demonstrate improved coagulation and decreased fibrinolytic vulnerability after exposure to CORM-2. METHODS: Normal plasma was anticoagulated with 0 to 0.1 U/mL unfractionated heparin or 0 to 1 mug/mL argatroban. Samples were subsequently exposed to 0 or 100 muM CORM-2 and activated with tissue factor. Additional samples with the same anticoagulant and CORM-2 exposure schema were incubated with 100 U/mL tissue-type plasminogen activator (tPA) to assess fibrinolytic vulnerability. Thrombelastographic data were collected until either clot strength stabilized or clot lysis occurred as appropriate. RESULTS: In the absence of tPA, CORM-2 significantly increased the velocity of clot growth in heparin (75%) and argatroban-exposed (40%) samples. Clot strength was also significantly increased in heparin (69%) and argatroban-exposed (72%) samples. In the presence of tPA, CORM-2-treated samples had even greater (94%-731%) increases in velocity of growth and strength after exposure to either anticoagulant and significantly increased clot lysis time (103%-200%). CONCLUSIONS: CORM-2 exposure resulted in faster-growing, stronger, longer-lived thrombi after anticoagulation with heparin or argatroban. Additional preclinical investigation is warranted to determine whether CORM-2 administration will be useful in attenuating bleeding complications associated with thromboprophylaxis.
机译:背景:最近已证明,一氧化碳释放分子(三羰基二氯钌[II]二聚体; CORM-2)可增强凝血功能,并减弱正常和血友病人血浆中对纤维蛋白溶解的脆弱性。我们测试了以下假设,即用肝素或阿加曲班抗凝的血浆在暴露于CORM-2后将显示出改善的凝血功能并降低纤溶敏感性。方法:正常血浆用0至0.1 U / mL普通肝素或0至1杯/ mL阿加曲班抗凝。随后将样品暴露于0或100μMCORM-2并用组织因子激活。将具有相同抗凝剂和CORM-2暴露方案的其他样品与100 U / mL组织型纤溶酶原激活剂(tPA)孵育,以评估纤溶酶的脆弱性。收集血栓弹力图数据,直到适当地凝块强度稳定或发生凝块溶解为止。结果:在没有tPA的情况下,CORM-2显着提高了肝素(75%)和阿加曲班暴露(40%)样品中的血块生长速度。肝素(69%)和暴露于阿加曲班的样本(72%)的血凝强度也显着提高。在存在tPA的情况下,接受任何一种抗凝剂后,经CORM-2处理的样品在生长速度和强度上的增加甚至更大(94%-731%),并且血块溶解时间也大大增加(103%-200%)。结论:肝素或阿加曲班抗凝后,CORM-2暴露导致血栓生长更快,更结实,寿命更长。有必要进行额外的临床前研究以确定CORM-2给药是否可用于减轻与血栓预防相关的出血并发症。

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