Molecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and Experiments
Abstract Despite the common use of thrombolytic drugs, especially in stroke treatment, there are many conflicting studies on factors affecting fibrinolysis. Because of the complexity of the fibrinolytic system, mathematical models closely tied with experiments can be used to understand relationships...
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2017-08-01
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Online Access: | https://doi.org/10.1038/s41598-017-06383-w |
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doaj-d863aaf2dbc74d158f8a400faec977032020-12-08T00:37:45ZengNature Publishing GroupScientific Reports2045-23222017-08-017111110.1038/s41598-017-06383-wMolecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and ExperimentsBrittany E. Bannish0Irina N. Chernysh1James P. Keener2Aaron L. Fogelson3John W. Weisel4University of Central Oklahoma, Department of Mathematics and StatisticsUniversity of Pennsylvania School of Medicine, Department of Cell and Developmental BiologyUniversity of Utah, Departments of Mathematics and BioengineeringUniversity of Utah, Departments of Mathematics and BioengineeringUniversity of Pennsylvania School of Medicine, Department of Cell and Developmental BiologyAbstract Despite the common use of thrombolytic drugs, especially in stroke treatment, there are many conflicting studies on factors affecting fibrinolysis. Because of the complexity of the fibrinolytic system, mathematical models closely tied with experiments can be used to understand relationships within the system. When tPA is introduced at the clot or thrombus edge, lysis proceeds as a front. We developed a multiscale model of fibrinolysis that includes the main chemical reactions: the microscale model represents a single fiber cross-section; the macroscale model represents a three-dimensional fibrin clot. The model successfully simulates the spatial and temporal locations of all components and elucidates how lysis rates are determined by the interplay between the number of tPA molecules in the system and clot structure. We used the model to identify kinetic conditions necessary for fibrinolysis to proceed as a front. We found that plasmin regulates the local concentration of tPA through forced unbinding via degradation of fibrin and tPA release. The mechanism of action of tPA is affected by the number of molecules present with respect to fibrin fibers. The physical mechanism of plasmin action (crawling) and avoidance of inhibition is defined. Many of these new findings have significant implications for thrombolytic treatment.https://doi.org/10.1038/s41598-017-06383-w |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Brittany E. Bannish Irina N. Chernysh James P. Keener Aaron L. Fogelson John W. Weisel |
spellingShingle |
Brittany E. Bannish Irina N. Chernysh James P. Keener Aaron L. Fogelson John W. Weisel Molecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and Experiments Scientific Reports |
author_facet |
Brittany E. Bannish Irina N. Chernysh James P. Keener Aaron L. Fogelson John W. Weisel |
author_sort |
Brittany E. Bannish |
title |
Molecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and Experiments |
title_short |
Molecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and Experiments |
title_full |
Molecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and Experiments |
title_fullStr |
Molecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and Experiments |
title_full_unstemmed |
Molecular and Physical Mechanisms of Fibrinolysis and Thrombolysis from Mathematical Modeling and Experiments |
title_sort |
molecular and physical mechanisms of fibrinolysis and thrombolysis from mathematical modeling and experiments |
publisher |
Nature Publishing Group |
series |
Scientific Reports |
issn |
2045-2322 |
publishDate |
2017-08-01 |
description |
Abstract Despite the common use of thrombolytic drugs, especially in stroke treatment, there are many conflicting studies on factors affecting fibrinolysis. Because of the complexity of the fibrinolytic system, mathematical models closely tied with experiments can be used to understand relationships within the system. When tPA is introduced at the clot or thrombus edge, lysis proceeds as a front. We developed a multiscale model of fibrinolysis that includes the main chemical reactions: the microscale model represents a single fiber cross-section; the macroscale model represents a three-dimensional fibrin clot. The model successfully simulates the spatial and temporal locations of all components and elucidates how lysis rates are determined by the interplay between the number of tPA molecules in the system and clot structure. We used the model to identify kinetic conditions necessary for fibrinolysis to proceed as a front. We found that plasmin regulates the local concentration of tPA through forced unbinding via degradation of fibrin and tPA release. The mechanism of action of tPA is affected by the number of molecules present with respect to fibrin fibers. The physical mechanism of plasmin action (crawling) and avoidance of inhibition is defined. Many of these new findings have significant implications for thrombolytic treatment. |
url |
https://doi.org/10.1038/s41598-017-06383-w |
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