使用新型改良凝血酶生成试验对正常犬和血友病犬血浆中的凝血进行整体测量——体内外实验证明

Global measurement of coagulation in plasma from normal and haemophilia dogs using a novel modified thrombin generation test - Demonstrated in vitro and ex vivo.

作者信息

Madsen Daniel Elenius, Nichols Timothy C, Merricks Elizabeth P, Waters Emily K, Wiinberg Bo

机构信息

Translational Haemophilia Pharmacology, Global Research, Novo Nordisk A/S, Måløv, Denmark.

Department of Pathology and Laboratory Medicine, University of North Carolina, Chapel Hill, North Carolina, United States of America.

出版信息

PLoS One. 2017 Apr 6;12(4):e0175030. doi: 10.1371/journal.pone.0175030. eCollection 2017.

DOI:10.1371/journal.pone.0175030

PMID:28384182

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5383133/

Abstract

INTRODUCTION

Canine models of severe haemophilia resemble their human equivalents both regarding clinical bleeding phenotype and response to treatment. Therefore pre-clinical studies in haemophilia dogs have allowed researchers to make valuable translational predictions regarding the potency and efficacy of new anti-haemophilia drugs (AHDs) in humans. To refine in vivo experiments and reduce number of animals, such translational studies are ideally preceded by in vitro prediction of compound efficacy using a plasma based global coagulation method. One such widely used method is the thrombin generation test (TGT). Unfortunately, commercially available TGTs are incapable of distinguishing between normal and haemophilia canine plasma, and therefore in vitro prediction using TGT has so far not been possible in canine plasma material.

AIM

Establish a modified TGT capable of: 1) distinguishing between normal and haemophilia canine plasma, 2) monitoring correlation between canine plasma levels of coagulation factor VIII (FVIII) and IX (FIX) and thrombin generation, 3) assessing for agreement between compound activity and thrombin generation in ex vivo samples.

METHODS

A modified TGT assay was established where coagulation was triggered using a commercially available activated partial thromboplastin time reagent.

RESULTS

With the modified TGT a significant difference was observed in thrombin generation between normal and haemophilia canine plasma. A dose dependent thrombin generation was observed when assessing haemophilia A and B plasma spiked with dilution series of FVIII and FIX, respectively. Correlation between FVIII activity and thrombin generation was observed when analyzing samples from haemophilia A dogs dosed with canine FVIII. Limit of detection was 0.1% (v/v) FVIII or FIX.

CONCLUSION

A novel modified TGT suitable for monitoring and prediction of replacement therapy efficacy in plasma from haemophilia A and B dogs was established.

摘要

引言

重度血友病犬模型在临床出血表型和对治疗的反应方面与人类血友病患者相似。因此，针对血友病犬的临床前研究使研究人员能够对新型抗血友病药物（AHDs）在人类中的效力和疗效做出有价值的转化预测。为了优化体内实验并减少动物数量，此类转化研究理想情况下应以基于血浆的整体凝血方法对化合物疗效进行体外预测为先导。一种广泛使用的此类方法是凝血酶生成试验（TGT）。不幸的是，市售的TGT无法区分正常犬血浆和血友病犬血浆，因此迄今为止，无法在犬血浆材料中使用TGT进行体外预测。

目的

建立一种改良的TGT，能够：1）区分正常犬血浆和血友病犬血浆；2）监测犬血浆中凝血因子VIII（FVIII）和IX（FIX）水平与凝血酶生成之间的相关性；3）评估离体样品中化合物活性与凝血酶生成之间的一致性。

方法

建立了一种改良的TGT测定法，使用市售的活化部分凝血活酶时间试剂触发凝血。

结果

使用改良的TGT，观察到正常犬血浆和血友病犬血浆之间的凝血酶生成存在显著差异。分别评估用FVIII和FIX稀释系列加标的血友病A和B血浆时，观察到剂量依赖性凝血酶生成。分析用犬FVIII给药的血友病A犬的样品时，观察到FVIII活性与凝血酶生成之间的相关性。检测限为0.1%（v/v）FVIII或FIX。