Combination Therapy Accelerates Diabetic Wound Closure

BACKGROUND: Non-healing foot ulcers are the most common cause of non-traumatic amputation and hospitalization amongst diabetics in the developed world. Impaired wound neovascularization perpetuates a cycle of dysfunctional tissue repair and regeneration. Evidence implicates defective mobilization of...

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Autores principales: Allen Jr., Robert J., Soares, Marc A., Haberman, Ilyse D., Szpalski, Caroline, Schachar, Jeffrey, Lin, Clarence D., Nguyen, Phuong D., Saadeh, Pierre B., Warren, Stephen M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3961401/
https://www.ncbi.nlm.nih.gov/pubmed/24651576
http://dx.doi.org/10.1371/journal.pone.0092667
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author Allen Jr., Robert J.
Soares, Marc A.
Haberman, Ilyse D.
Szpalski, Caroline
Schachar, Jeffrey
Lin, Clarence D.
Nguyen, Phuong D.
Saadeh, Pierre B.
Warren, Stephen M.
author_facet Allen Jr., Robert J.
Soares, Marc A.
Haberman, Ilyse D.
Szpalski, Caroline
Schachar, Jeffrey
Lin, Clarence D.
Nguyen, Phuong D.
Saadeh, Pierre B.
Warren, Stephen M.
author_sort Allen Jr., Robert J.
collection PubMed
description BACKGROUND: Non-healing foot ulcers are the most common cause of non-traumatic amputation and hospitalization amongst diabetics in the developed world. Impaired wound neovascularization perpetuates a cycle of dysfunctional tissue repair and regeneration. Evidence implicates defective mobilization of marrow-derived progenitor cells (PCs) as a fundamental cause of impaired diabetic neovascularization. Currently, there are no FDA-approved therapies to address this defect. Here we report an endogenous PC strategy to improve diabetic wound neovascularization and closure through a combination therapy of AMD3100, which mobilizes marrow-derived PCs by competitively binding to the cell surface CXCR4 receptor, and PDGF-BB, which is a protein known to enhance cell growth, progenitor cell migration and angiogenesis. METHODS AND RESULTS: Wounded mice were assigned to 1 of 5 experimental arms (n = 8/arm): saline treated wild-type, saline treated diabetic, AMD3100 treated diabetic, PDGF-BB treated diabetic, and AMD3100/PDGF-BB treated diabetic. Circulating PC number and wound vascularity were analyzed for each group (n = 8/group). Cellular function was assessed in the presence of AMD3100. Using a validated preclinical model of type II diabetic wound healing, we show that AMD3100 therapy (10 mg/kg; i.p. daily) alone can rescue diabetes-specific defects in PC mobilization, but cannot restore normal wound neovascularization. Through further investigation, we demonstrate an acquired trafficking-defect within AMD3100-treated diabetic PCs that can be rescued by PDGF-BB (2 μg; topical) supplementation within the wound environment. Finally, we determine that combination therapy restores diabetic wound neovascularization and accelerates time to wound closure by 40%. CONCLUSIONS: Combination AMD3100 and PDGF-BB therapy synergistically improves BM PC mobilization and trafficking, resulting in significantly improved diabetic wound closure and neovascularization. The success of this endogenous, cell-based strategy to improve diabetic wound healing using FDA-approved therapies is inherently translatable.
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spelling pubmed-39614012014-03-24 Combination Therapy Accelerates Diabetic Wound Closure Allen Jr., Robert J. Soares, Marc A. Haberman, Ilyse D. Szpalski, Caroline Schachar, Jeffrey Lin, Clarence D. Nguyen, Phuong D. Saadeh, Pierre B. Warren, Stephen M. PLoS One Research Article BACKGROUND: Non-healing foot ulcers are the most common cause of non-traumatic amputation and hospitalization amongst diabetics in the developed world. Impaired wound neovascularization perpetuates a cycle of dysfunctional tissue repair and regeneration. Evidence implicates defective mobilization of marrow-derived progenitor cells (PCs) as a fundamental cause of impaired diabetic neovascularization. Currently, there are no FDA-approved therapies to address this defect. Here we report an endogenous PC strategy to improve diabetic wound neovascularization and closure through a combination therapy of AMD3100, which mobilizes marrow-derived PCs by competitively binding to the cell surface CXCR4 receptor, and PDGF-BB, which is a protein known to enhance cell growth, progenitor cell migration and angiogenesis. METHODS AND RESULTS: Wounded mice were assigned to 1 of 5 experimental arms (n = 8/arm): saline treated wild-type, saline treated diabetic, AMD3100 treated diabetic, PDGF-BB treated diabetic, and AMD3100/PDGF-BB treated diabetic. Circulating PC number and wound vascularity were analyzed for each group (n = 8/group). Cellular function was assessed in the presence of AMD3100. Using a validated preclinical model of type II diabetic wound healing, we show that AMD3100 therapy (10 mg/kg; i.p. daily) alone can rescue diabetes-specific defects in PC mobilization, but cannot restore normal wound neovascularization. Through further investigation, we demonstrate an acquired trafficking-defect within AMD3100-treated diabetic PCs that can be rescued by PDGF-BB (2 μg; topical) supplementation within the wound environment. Finally, we determine that combination therapy restores diabetic wound neovascularization and accelerates time to wound closure by 40%. CONCLUSIONS: Combination AMD3100 and PDGF-BB therapy synergistically improves BM PC mobilization and trafficking, resulting in significantly improved diabetic wound closure and neovascularization. The success of this endogenous, cell-based strategy to improve diabetic wound healing using FDA-approved therapies is inherently translatable. Public Library of Science 2014-03-20 /pmc/articles/PMC3961401/ /pubmed/24651576 http://dx.doi.org/10.1371/journal.pone.0092667 Text en © 2014 Allen, et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Allen Jr., Robert J.
Soares, Marc A.
Haberman, Ilyse D.
Szpalski, Caroline
Schachar, Jeffrey
Lin, Clarence D.
Nguyen, Phuong D.
Saadeh, Pierre B.
Warren, Stephen M.
Combination Therapy Accelerates Diabetic Wound Closure
title Combination Therapy Accelerates Diabetic Wound Closure
title_full Combination Therapy Accelerates Diabetic Wound Closure
title_fullStr Combination Therapy Accelerates Diabetic Wound Closure
title_full_unstemmed Combination Therapy Accelerates Diabetic Wound Closure
title_short Combination Therapy Accelerates Diabetic Wound Closure
title_sort combination therapy accelerates diabetic wound closure
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3961401/
https://www.ncbi.nlm.nih.gov/pubmed/24651576
http://dx.doi.org/10.1371/journal.pone.0092667
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