Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study

Fibrinolytic therapy of venous thromboembolism (VTE) is increasingly utilized, yet limited knowledge is available regarding in vivo mechanisms that govern fibrinolytic efficacy. In particular, it is unknown how age-dependent thrombus organization limits direct blood contact with fibrin, the target o...

Descripción completa

Detalles Bibliográficos
Autores principales: Stein-Merlob, Ashley F., Kessinger, Chase W., Erdem, S. Sibel, Zelada, Henry, Hilderbrand, Scott A., Lin, Charles P., Tearney, Guillermo J., Jaff, Michael R., Reed, Guy L., Henke, Peter K., McCarthy, Jason R., Jaffer, Farouc A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2015
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4615735/
https://www.ncbi.nlm.nih.gov/pubmed/26516370
http://dx.doi.org/10.7150/thno.12494
_version_ 1782396507284045824
author Stein-Merlob, Ashley F.
Kessinger, Chase W.
Erdem, S. Sibel
Zelada, Henry
Hilderbrand, Scott A.
Lin, Charles P.
Tearney, Guillermo J.
Jaff, Michael R.
Reed, Guy L.
Henke, Peter K.
McCarthy, Jason R.
Jaffer, Farouc A.
author_facet Stein-Merlob, Ashley F.
Kessinger, Chase W.
Erdem, S. Sibel
Zelada, Henry
Hilderbrand, Scott A.
Lin, Charles P.
Tearney, Guillermo J.
Jaff, Michael R.
Reed, Guy L.
Henke, Peter K.
McCarthy, Jason R.
Jaffer, Farouc A.
author_sort Stein-Merlob, Ashley F.
collection PubMed
description Fibrinolytic therapy of venous thromboembolism (VTE) is increasingly utilized, yet limited knowledge is available regarding in vivo mechanisms that govern fibrinolytic efficacy. In particular, it is unknown how age-dependent thrombus organization limits direct blood contact with fibrin, the target of blood-based fibrinolytic agents. Utilizing high-resolution in vivo optical molecular imaging with FTP11, a near-infrared fluorescence (NIRF) fibrin-specific reporter, here we investigated the in vivo interrelationships of blood accessibility to fibrin, thrombus age, thrombus neoendothelialization, and fibrinolysis in murine venous thrombosis (VT). In both stasis VT and non-stasis VT, NIRF microscopy showed that FTP11 fibrin binding was thrombus age-dependent. FTP11 localized to the luminal surface of early-stage VT, but only minimally to subacute VT (p<0.001). Transmission electron microscopy of early stage VT revealed direct blood cell contact with luminal fibrin-rich surfaces. In contrast, subacute VT exhibited an encasing CD31+ neoendothelial layer that limited blood cell contact with thrombus fibrin in both VT models. Next we developed a theranostic strategy to predict fibrinolytic efficacy based on the in vivo fibrin accessibility to blood NIRF signal. Mice with variably aged VT underwent FTP11 injection and intravital microscopy (IVM), followed by tissue plasminogen activator infusion to induce VT fibrinolysis. Fibrin molecular IVM revealed that early stage VT, but not subacute VT, bound FTP11 (p<0.05), and experienced higher rates of fibrinolysis and total fibrinolysis (p<0.05 vs. subacute VT). Before fibrinolysis, the baseline FTP11 NIRF signal predicted the net fibrinolysis at 60 minutes (p<0.001). Taken together, these data provide novel insights into the temporal evolution of VT and its susceptibility to therapeutic fibrinolysis. Fibrin molecular imaging may provide a theranostic strategy to identify venous thrombi amenable to fibrinolytic therapies.
format Online
Article
Text
id pubmed-4615735
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-46157352015-10-29 Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study Stein-Merlob, Ashley F. Kessinger, Chase W. Erdem, S. Sibel Zelada, Henry Hilderbrand, Scott A. Lin, Charles P. Tearney, Guillermo J. Jaff, Michael R. Reed, Guy L. Henke, Peter K. McCarthy, Jason R. Jaffer, Farouc A. Theranostics Research Paper Fibrinolytic therapy of venous thromboembolism (VTE) is increasingly utilized, yet limited knowledge is available regarding in vivo mechanisms that govern fibrinolytic efficacy. In particular, it is unknown how age-dependent thrombus organization limits direct blood contact with fibrin, the target of blood-based fibrinolytic agents. Utilizing high-resolution in vivo optical molecular imaging with FTP11, a near-infrared fluorescence (NIRF) fibrin-specific reporter, here we investigated the in vivo interrelationships of blood accessibility to fibrin, thrombus age, thrombus neoendothelialization, and fibrinolysis in murine venous thrombosis (VT). In both stasis VT and non-stasis VT, NIRF microscopy showed that FTP11 fibrin binding was thrombus age-dependent. FTP11 localized to the luminal surface of early-stage VT, but only minimally to subacute VT (p<0.001). Transmission electron microscopy of early stage VT revealed direct blood cell contact with luminal fibrin-rich surfaces. In contrast, subacute VT exhibited an encasing CD31+ neoendothelial layer that limited blood cell contact with thrombus fibrin in both VT models. Next we developed a theranostic strategy to predict fibrinolytic efficacy based on the in vivo fibrin accessibility to blood NIRF signal. Mice with variably aged VT underwent FTP11 injection and intravital microscopy (IVM), followed by tissue plasminogen activator infusion to induce VT fibrinolysis. Fibrin molecular IVM revealed that early stage VT, but not subacute VT, bound FTP11 (p<0.05), and experienced higher rates of fibrinolysis and total fibrinolysis (p<0.05 vs. subacute VT). Before fibrinolysis, the baseline FTP11 NIRF signal predicted the net fibrinolysis at 60 minutes (p<0.001). Taken together, these data provide novel insights into the temporal evolution of VT and its susceptibility to therapeutic fibrinolysis. Fibrin molecular imaging may provide a theranostic strategy to identify venous thrombi amenable to fibrinolytic therapies. Ivyspring International Publisher 2015-09-13 /pmc/articles/PMC4615735/ /pubmed/26516370 http://dx.doi.org/10.7150/thno.12494 Text en © 2015 Ivyspring International Publisher. Reproduction is permitted for personal, noncommercial use, provided that the article is in whole, unmodified, and properly cited. See http://ivyspring.com/terms for terms and conditions.
spellingShingle Research Paper
Stein-Merlob, Ashley F.
Kessinger, Chase W.
Erdem, S. Sibel
Zelada, Henry
Hilderbrand, Scott A.
Lin, Charles P.
Tearney, Guillermo J.
Jaff, Michael R.
Reed, Guy L.
Henke, Peter K.
McCarthy, Jason R.
Jaffer, Farouc A.
Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study
title Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study
title_full Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study
title_fullStr Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study
title_full_unstemmed Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study
title_short Blood Accessibility to Fibrin in Venous Thrombosis is Thrombus Age-Dependent and Predicts Fibrinolytic Efficacy: An In Vivo Fibrin Molecular Imaging Study
title_sort blood accessibility to fibrin in venous thrombosis is thrombus age-dependent and predicts fibrinolytic efficacy: an in vivo fibrin molecular imaging study
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4615735/
https://www.ncbi.nlm.nih.gov/pubmed/26516370
http://dx.doi.org/10.7150/thno.12494
work_keys_str_mv AT steinmerlobashleyf bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT kessingerchasew bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT erdemssibel bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT zeladahenry bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT hilderbrandscotta bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT lincharlesp bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT tearneyguillermoj bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT jaffmichaelr bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT reedguyl bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT henkepeterk bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT mccarthyjasonr bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy
AT jafferfarouca bloodaccessibilitytofibrininvenousthrombosisisthrombusagedependentandpredictsfibrinolyticefficacyaninvivofibrinmolecularimagingstudy

Ejemplares similares