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Quantitative Systems Pharmacology Model to Predict the Effects of Commonly Used Anticoagulants on the Human Coagulation Network

机译:定量系统药理模型预测常用抗凝剂对人凝血网络的影响

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Warfarin is the anticoagulant of choice for venous thromboembolism (VTE) treatment, although its suppression of the endogenous clot?¢????dissolution complex APC:PS may ultimately lead to longer time?¢????to?¢????clot dissolution profiles, resulting in increased risk of re?¢????thrombosis. This detrimental effect might not occur during VTE treatment using other anticoagulants, such as rivaroxaban or enoxaparin, given their different mechanisms of action within the coagulation network. A quantitative systems pharmacology model was developed describing the coagulation network to monitor clotting factor levels under warfarin, enoxaparin, and rivaroxaban treatment. The model allowed for estimation of all factor rate constants and production rates. Predictions of individual coagulation factor time courses under steady?¢????state warfarin, enoxaparin, and rivaroxaban treatment reflected the suppression of protein C and protein S under warfarin compared to rivaroxaban and enoxaparin. The model may be used as a tool during clinical practice to predict effects of anticoagulants on individual clotting factor time courses and optimize antithrombotic therapy.
机译:华法林是静脉血栓栓塞(VTE)治疗的首选抗凝剂,尽管它抑制内源性血凝块溶解复合物APC:PS可能最终导致更长的时间。凝血溶解曲线,导致再次形成血栓的风险增加。考虑到它们在凝血网络中的不同作用机制,在使用其他抗凝剂(如利伐沙班或依诺肝素)进行VTE治疗期间,可能不会发生这种有害作用。建立了描述凝血网络的定量系统药理模型,以监测华法林,依诺肝素和利伐沙班治疗下的凝血因子水平。该模型允许估算所有因子速率常数和生产率。在稳态华法林,依诺肝素和利伐沙班治疗下,各个凝血因子时间进程的预测反映了与利伐沙班和依诺肝素相比,华法林对蛋白C和S的抑制作用。该模型可在临床实践中用作预测抗凝剂对个体凝血因子时间进程的影响并优化抗血栓治疗的工具。

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