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凝血酶抑制剂与地塞米松联合使用可预防大鼠实验性弥散性血管内凝血的发生。

A combination of a thrombin inhibitor and dexamethasone prevents the development of experimental disseminated intravascular coagulation in rats.

作者信息

Elg Margareta, Gustafsson David

机构信息

Department of Integrative Pharmacology, AstraZeneca R&D Mölndal, Mölndal, Sweden.

出版信息

Thromb Res. 2006;117(4):429-37. doi: 10.1016/j.thromres.2005.03.014.

DOI:10.1016/j.thromres.2005.03.014
PMID:15869787
Abstract

INTRODUCTION

Disseminated intravascular coagulation (DIC) is a serious and potentially lethal complication of severe sepsis. DIC is characterised primarily by widespread platelet aggregation and fibrin deposition, followed by consumption of platelets, coagulation factors, and inhibitors. The aim of the study was to evaluate the efficacy of the active-site thrombin inhibitor melagatran, the active form of the oral direct thrombin inhibitor ximelagatran, in reducing fibrinogen and platelet consumption in blood and fibrin deposition in organs, in an experimental endotoxinaemia rat model.

MATERIALS AND METHODS

In this model, DIC was induced by an intravenous injection of endotoxin (1 mg/kg). Melagatran was compared with unfractionated heparin and the synthetic glucocorticoid analogue dexamethasone. Animals were divided into 16 treatment groups in which high and low doses of each agent were tested alone and in combination with melagatran.

RESULTS

Fibrinogen consumption was reduced by melagatran, dexamethasone, and heparin, and was completely prevented by melagatran in combination with dexamethasone. Platelet consumption was partially reduced by melagatran, unfractionated heparin, and dexamethasone, but complete protection was observed only with melagatran in combination with dexamethasone. Melagatran in combination with dexamethasone or heparin protected the liver and spleen from fibrin deposition.

CONCLUSION

In this experimental DIC rat model, the direct thrombin inhibitor melagatran given together with dexamethasone protected against the consequences of activated haemostasis.

摘要

引言

弥散性血管内凝血(DIC)是严重脓毒症的一种严重且可能致命的并发症。DIC的主要特征是广泛的血小板聚集和纤维蛋白沉积,随后是血小板、凝血因子和抑制剂的消耗。本研究的目的是在实验性内毒素血症大鼠模型中,评估活性位点凝血酶抑制剂美拉加群(口服直接凝血酶抑制剂希美加群的活性形式)在减少血液中纤维蛋白原和血小板消耗以及器官中纤维蛋白沉积方面的疗效。

材料与方法

在该模型中,通过静脉注射内毒素(1毫克/千克)诱导DIC。将美拉加群与普通肝素和合成糖皮质激素类似物地塞米松进行比较。动物被分为16个治疗组,分别单独测试每种药物的高剂量和低剂量,并与美拉加群联合测试。

结果

美拉加群、地塞米松和肝素均可减少纤维蛋白原的消耗,美拉加群与地塞米松联合使用可完全阻止纤维蛋白原的消耗。美拉加群、普通肝素和地塞米松均可部分减少血小板的消耗,但仅美拉加群与地塞米松联合使用可实现完全保护。美拉加群与地塞米松或肝素联合使用可保护肝脏和脾脏免受纤维蛋白沉积。

结论

在这个实验性DIC大鼠模型中,直接凝血酶抑制剂美拉加群与地塞米松联合使用可预防激活的止血所带来的后果。

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