Abstract

A highly reduced extrinsic pathway coagulation model (8 ODEs) under flow considered a thin 15-micron platelet layer where transport limitations were largely negligible (except for fibrinogen) and where cofactors (FVIIa, FV, FVIII) were not rate-limiting. By including thrombin feedback activation of FXI and the antithrombin-I activities of fibrin, the model accurately simulated measured fibrin formation and thrombin fluxes. Using this reduced model, we conducted 10,000 Monte Carlo (MC) simulations for ±50% variation of 5 plasma zymogens and 2 fibrin binding sites for thrombin. A sensitivity analysis of zymogen concentrations indicated that FIX activity most influenced thrombin generation, a result expected from hemophilia A and B. Averaging all MC simulations confirmed both the mean and standard deviation of measured fibrin generation on 1 tissue factor (TF) molecule per μm2. Across all simulations, free thrombin in the layer ranged from 20 to 300 nM (mean: 50 nM). The top 2% of simulations that produced maximal fibrin were dominated by conditions with low antithrombin-I activity (decreased weak and strong sites) and high FIX concentration. In contrast, the bottom 2% of simulations that produced minimal fibrin were dominated by low FIX and FX. The percent reduction of fibrin by an ideal FXIa inhibitor (FXI = 0) ranged from 71% fibrin reduction in the top 2% of MC simulations to only 34% fibrin reduction in the bottom 2% of MC simulations. Thus, the antithrombotic potency of FXIa inhibitors may vary depending on normal ranges of zymogen concentrations. This reduced model allowed efficient multivariable sensitivity analysis.

Highlights

  • Blood clotting occurs under flow conditions in many circumstances of hemostasis or intravascular thrombosis

  • We explored the sensitivity of an extrinsic pathway model for a 15-micron film that was previously shown to simulate fibrin formation dynamics and thrombin generation dynamics

  • 3 parameters were adjusted from literature to fit the measured TAT, F1.2 and fibrin generation data (± GPRP)

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Summary

Introduction

Blood clotting occurs under flow conditions in many circumstances of hemostasis or intravascular thrombosis. When tissue factor is exposed to the blood the coagulation cascade is triggered, resulting in the eventual generation of thrombin and the polymerization of fibrin. The complexity is increased by the presence of flow, the participation of platelets. Multivariable sensitivity of reduced model of coagulation under flow in clot growth, and various strong couplings and feedbacks [4,5,6]. The further goal of multiscale modeling seeks to deploy complex vascular flows with realistic models of platelet signaling and coagulation function [8,9,10], all of which is extremely demanding from a computation point of view. Reduced models offer advantages in bridging scales and in handing 3D coupled reaction-diffusion-convection problems

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