Laboratory Testing for Fibrinogen Disorders: From Routine Investigations to Research Studies.

IF 3.6 2区 医学 Q2 HEMATOLOGY
Anetta Undas
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Abstract

Congenital and acquired fibrinogen disorders often have heterogeneous clinical phenotypes and are challenging from a laboratory perspective. Fibrinogen determination using the Clauss method remains the gold standard, while the reproducibility and significance of the thrombin time and the reptilase time are limited. Molecular testing for causative mutations in fibrinogen genes is now recommended to confirm the diagnosis of congenital fibrinogen disorders. Research assays are used to evaluate alterations to fibrin formation and properties of plasma and purified fibrinogen-derived clots, characterized by fiber thickness, the number of branches, and pore sizes. Fibrin clot permeability (permeation, porosity) using a hydrostatic pressure system represents the most commonly used method for evaluating fibrin network density. Reduced clot permeability, which denotes the reduced size of an average pore in the network, results in tighter fibrin networks, typically associated with impaired susceptibility to lysis, leading to a thrombotic tendency. Biophysical properties of fibrin clots are largely assessed using rheometry, with atomic force microscopy and nanorheology being increasingly used in disease states. Thromboelastography and thromboelastometry, a simple modification of rheometry, have been used, mainly in intensive care units, for more than 50 years. Given growing evidence for altered fibrin clot properties in diseases with elevated risk of venous and arterial thromboembolism and in some bleeding disorders, further work on standardization and validation of the assessment of fibrin clot characteristics is needed. This review summarizes the current methods used to evaluate fibrinogen abnormalities in both diagnostic and research laboratories.

纤维蛋白原紊乱的实验室检测:从常规检查到研究调查。
先天性和后天性纤维蛋白原紊乱通常具有不同的临床表型,从实验室角度来看具有挑战性。使用克劳斯法测定纤维蛋白原仍是金标准,而凝血酶时间和爬行酶时间的可重复性和意义有限。目前建议进行纤维蛋白原基因致病突变的分子检测,以确诊先天性纤维蛋白原紊乱。研究测定用于评估纤维蛋白形成的改变以及血浆和纯化纤维蛋白原衍生凝块的特性,其特点是纤维厚度、分支数量和孔隙大小。使用静水压系统检测纤维蛋白凝块渗透性(渗透、孔隙率)是评估纤维蛋白网络密度最常用的方法。凝块通透性降低表示网络中平均孔径减小,会导致纤维蛋白网络更紧密,通常与溶解敏感性降低有关,从而导致血栓形成倾向。纤维蛋白凝块的生物物理特性主要通过流变仪进行评估,原子力显微镜和纳米流变学正越来越多地用于疾病状态。血栓弹性成像和血栓弹性测量是流变仪的一种简单改进,主要用于重症监护病房,已有 50 多年的历史。鉴于越来越多的证据表明,在静脉和动脉血栓栓塞风险升高的疾病以及某些出血性疾病中,纤维蛋白凝块的特性会发生改变,因此需要进一步开展标准化工作,并验证纤维蛋白凝块特性的评估。本综述总结了目前诊断和研究实验室用于评估纤维蛋白原异常的方法。
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来源期刊
Seminars in thrombosis and hemostasis
Seminars in thrombosis and hemostasis 医学-外周血管病
CiteScore
8.80
自引率
21.10%
发文量
132
审稿时长
6-12 weeks
期刊介绍: Seminars in Thrombosis and Hemostasis is a topic driven review journal that focuses on all issues relating to hemostatic and thrombotic disorders. As one of the premiere review journals in the field, Seminars in Thrombosis and Hemostasis serves as a comprehensive forum for important advances in clinical and laboratory diagnosis and therapeutic interventions. The journal also publishes peer reviewed original research papers. Seminars offers an informed perspective on today''s pivotal issues, including hemophilia A & B, thrombophilia, gene therapy, venous and arterial thrombosis, von Willebrand disease, vascular disorders and thromboembolic diseases. Attention is also given to the latest developments in pharmaceutical drugs along with treatment and current management techniques. The journal also frequently publishes sponsored supplements to further highlight emerging trends in the field.
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