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体外添加血浆代用品后的血栓弹力图全血凝块形成:纤维蛋白原浓缩物对诱导性凝血病的改善作用

Thrombelastographic whole blood clot formation after ex vivo addition of plasma substitutes: improvements of the induced coagulopathy with fibrinogen concentrate.

作者信息

Fenger-Eriksen C, Anker-Møller E, Heslop J, Ingerslev J, Sørensen B

机构信息

Department of Anaesthesiology, Aarhus University Hospital, Aarhus Sygehus, Denmark.

出版信息

Br J Anaesth. 2005 Mar;94(3):324-9. doi: 10.1093/bja/aei052. Epub 2004 Dec 17.

Abstract

BACKGROUND

Plasma substitutes such as hydroxyethyl starch (HES) and various dextrans may compromise the haemostatic system, thereby causing potentially dangerous bleeding. Whilst several mechanisms have been advanced to explain the nature of the coagulopathy induced by this colloid, there has been comparably little interest in devising ways to optimize haemostasis after a relative colloid overdose.

METHODS

Real-time whole blood (WB) clot formation profiles were recorded using a thrombelastographic method employing activation with tissue factor. The coagulation tracings were transformed into dynamic velocity profiles of WB clot formation. WB from healthy individuals (n=20) was exposed to haemodilution of approximately 55% with isotonic saline, HES 200/0.5, HES 130/0.4, and dextran 70, respectively. Possible modalities for improvement of the induced coagulopathy were explored, in particular ex vivo addition of a fibrinogen concentrate.

RESULTS

WB coagulation profiles changed significantly with decreased clot strength, and a compromised propagation phase of clot formation. The duration of the initiation phase of WB coagulation was unchanged. No statistical differences were detected amongst the HES solutions and dextran 70. However, dextran 70 returned a more suppressed clot development and strength compared with the HES solutions. Ex vivo haemostatic addition of washed platelets (75 x 10(9) litre(-1)) and factor VIII (0.6 IU ml(-1)) produced insignificant changes in clot initiation, propagation, and in the clot strength. In contrast, ex vivo addition of a fibrinogen concentrate (1 g litre(-1)) improved the coagulopathy induced by all of the three individual plasma expanders tested.

CONCLUSION

Coagulopathy induced by haemodilution with either HES 200/0.5, HES 130/0.4, and dextran 70 may be improved by fibrinogen supplementation.

摘要

背景

血浆代用品如羟乙基淀粉(HES)和各种右旋糖酐可能会损害止血系统,从而导致潜在的危险出血。虽然已经提出了几种机制来解释这种胶体引起的凝血病的性质,但对于设计方法来优化相对胶体过量后的止血,人们的兴趣相对较少。

方法

使用组织因子激活的血栓弹力图方法记录全血(WB)实时凝血形成曲线。将凝血描记图转换为WB凝血形成的动态速度曲线。分别用等渗盐水、HES 200/0.5、HES 130/0.4和右旋糖酐70对健康个体(n = 20)的WB进行约55%的血液稀释。探索了改善诱导凝血病的可能方式,特别是在体外添加纤维蛋白原浓缩物。

结果

WB凝血曲线随凝血强度降低和凝血形成的传播阶段受损而发生显著变化。WB凝血起始阶段的持续时间未改变。在HES溶液和右旋糖酐70之间未检测到统计学差异。然而,与HES溶液相比,右旋糖酐70的凝血发展和强度受到更明显的抑制。体外添加洗涤血小板(75×10⁹升⁻¹)和因子VIII(0.6 IU毫升⁻¹)对凝血起始、传播和凝血强度产生的变化不显著。相比之下,体外添加纤维蛋白原浓缩物(1克升⁻¹)改善了所测试的三种单独血浆扩容剂诱导的凝血病。

结论

补充纤维蛋白原可改善用HES 200/0.5、HES 130/0.4和右旋糖酐70进行血液稀释诱导的凝血病。

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