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临床样本中微粒组织因子活性的测定:两种组织因子依赖性FXa生成测定方法的总结

Measurement of microparticle tissue factor activity in clinical samples: A summary of two tissue factor-dependent FXa generation assays.

作者信息

Hisada Yohei, Alexander Wyeth, Kasthuri Raj, Voorhees Peter, Mobarrez Fariborz, Taylor Angela, McNamara Coleen, Wallen Hakan, Witkowski Marco, Key Nigel S, Rauch Ursula, Mackman Nigel

机构信息

McAllister Heart Institute, Department of Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.

K.G. Jebsen Thrombosis Research and Expertise Center, University of Tromsø, Tromsø, Norway.

出版信息

Thromb Res. 2016 Mar;139:90-7. doi: 10.1016/j.thromres.2016.01.011. Epub 2016 Jan 18.

Abstract

Thrombosis is a leading cause of morbidity and mortality. Detection of a prothrombotic state using biomarkers would be of great benefit to identify patients at risk of thrombosis that would benefit from thromboprophylaxis. Tissue factor (TF) is a highly procoagulant protein that under normal conditions is not present in the blood. However, increased levels of TF in the blood in the form of microparticles (MPs) (also called extracellular vesicles) are observed under various pathological conditions. In this review, we will discuss studies that have measured MP-TF activity in a variety of diseases using two similar FXa generation assay. One of the most robust signals for MP-TF activity (16-26 fold higher than healthy controls) is observed in pancreatic cancer patients with venous thromboembolism. In this case, the TF+ MPs appear to be derived from the cancer cells. Surprisingly, cirrhosis and acute liver injury are associated with 17-fold and 38-fold increases in MP-TF activity, respectively. Based on mouse models, we speculate that the TF+ MPs are derived from hepatocytes. More modest increases are observed in patients with urinary tract infections (6-fold) and in a human endotoxemia model (9-fold) where monocytes are the likely source of the TF+ MPs. Finally, there is no increase in MP-TF activity in the majority of cardiovascular disease patients. These studies indicate that MP-TF activity may be a useful biomarker to identify patients with particular diseases that have an increased risk of thrombosis.

摘要

血栓形成是发病和死亡的主要原因。使用生物标志物检测血栓前状态对于识别有血栓形成风险且能从血栓预防中获益的患者将大有裨益。组织因子(TF)是一种高度促凝蛋白,在正常情况下不存在于血液中。然而,在各种病理条件下,可观察到血液中以微粒(MPs)(也称为细胞外囊泡)形式存在的TF水平升高。在本综述中,我们将讨论使用两种相似的FXa生成测定法测量多种疾病中MP-TF活性的研究。在患有静脉血栓栓塞的胰腺癌患者中观察到MP-TF活性最强的信号之一(比健康对照高16 - 26倍)。在这种情况下,TF + MPs似乎来源于癌细胞。令人惊讶的是,肝硬化和急性肝损伤分别与MP-TF活性增加17倍和38倍有关。基于小鼠模型,我们推测TF + MPs来源于肝细胞。在尿路感染患者(6倍)和人类内毒素血症模型(9倍)中观察到更为适度的增加,其中单核细胞可能是TF + MPs的来源。最后,大多数心血管疾病患者的MP-TF活性没有增加。这些研究表明,MP-TF活性可能是一种有用的生物标志物,用于识别具有血栓形成风险增加的特定疾病患者。

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