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纤维蛋白溶解的测定。

Measuring Fibrinolysis.

机构信息

Department of Biotherapeutics, National Institute for Biological Standards and Control, South Mimms, Herts, United Kingdom.

出版信息

Hamostaseologie. 2021 Feb;41(1):69-75. doi: 10.1055/a-1325-0268. Epub 2021 Feb 15.

DOI:10.1055/a-1325-0268
PMID:33588458
Abstract

Physiological fibrinolysis under normal conditions progresses slowly, in contrast to coagulation which is triggered rapidly to stop bleeding and defend against microbial invasion. Methods to detect fibrinolysis abnormalities are less simple and poorly standardized compared with common coagulation tests. Fibrinolysis can be accelerated by preparing euglobulin from plasma to reduce endogenous inhibitors, or by adding plasminogen activators to normal plasma. However, these manipulations complicate interpretation of results and diagnosis of a "fibrinolysis deficit." Many observational studies on antigen levels of fibrinolysis inhibitors, plasminogen activator inhibitor 1 or thrombin-activatable fibrinolysis inhibitor, zymogen or active enzyme have been published. However, conclusions are mixed and there are clear problems with harmonization of results. Viscoelastic methods have the advantage of being rapid and are used as point-of-care tests. They also work with whole blood, allowing the contribution of platelets to be explored. However, there are no agreed protocols for applying viscoelastic methods in acute care for the diagnosis of hyperfibrinolysis or to direct therapy. The emergence of SARS-CoV-2 and the dangers of associated coagulopathy provide new challenges. A common finding in hospitalized patients is high levels of D-dimer fibrin breakdown products, indicative of ongoing fibrinolysis. Well-established problems with D-dimer testing standardization signal that we should be cautious in using results from such tests as prognostic indicators or to target therapies.

摘要

在正常情况下,生理纤溶缓慢进展,与迅速触发以止血和抵御微生物入侵的凝血形成鲜明对比。与常见的凝血试验相比,检测纤溶异常的方法不那么简单,也没有得到很好的标准化。通过从血浆中制备优球蛋白来减少内源性抑制剂,或向正常血浆中添加纤溶酶原激活物,可以加速纤溶。然而,这些操作使结果的解释和“纤溶缺陷”的诊断变得复杂。已经发表了许多关于纤溶抑制剂、纤溶酶原激活物抑制剂 1 或凝血酶激活的纤溶抑制剂、酶原或活性酶的抗原水平的观察性研究。然而,结论不一,并且在结果的协调方面存在明显的问题。黏弹性方法的优点是快速,可作为即时检测方法使用。它们还可以与全血一起使用,从而可以探索血小板的贡献。然而,在急性护理中,没有用于诊断高纤溶或指导治疗的黏弹性方法应用的协议。SARS-CoV-2 的出现及其相关凝血障碍的危险带来了新的挑战。住院患者的一个常见发现是 D-二聚体纤维蛋白降解产物水平升高,表明持续纤溶。D-二聚体检测标准化的既定问题表明,我们应该谨慎使用这些测试结果作为预后指标或靶向治疗。

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