A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds

Introduction: Diabetes mellitus describes a dysregulation of glucose metabolism due to improper insulin secretion, reduced insulin efficacy or both. It is a well-known fact that diabetic patients are likely to suffer from impaired wound healing, as diabetes strongly affects tissue angiogenesis. Unti...

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Autores principales: Langer, Stefan, Beescho, Christian, Ring, Andrej, Dorfmann, Olivia, Steinau, Hans Ulrich, Spindler, Nick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: German Medical Science GMS Publishing House 2016
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4764794/
https://www.ncbi.nlm.nih.gov/pubmed/26955508
http://dx.doi.org/10.3205/iprs000088
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author Langer, Stefan
Beescho, Christian
Ring, Andrej
Dorfmann, Olivia
Steinau, Hans Ulrich
Spindler, Nick
author_facet Langer, Stefan
Beescho, Christian
Ring, Andrej
Dorfmann, Olivia
Steinau, Hans Ulrich
Spindler, Nick
author_sort Langer, Stefan
collection PubMed
description Introduction: Diabetes mellitus describes a dysregulation of glucose metabolism due to improper insulin secretion, reduced insulin efficacy or both. It is a well-known fact that diabetic patients are likely to suffer from impaired wound healing, as diabetes strongly affects tissue angiogenesis. Until now, no satisfying in vivo murine model has been established to analyze the dynamics of angiogenesis during diabetic wound healing. To help understand the pathophysiology of diabetes and its effect on angiogenesis, a novel in vivo murine model was established using the skinfold chamber in mice. Materials and Methods: Mutant diabetic mice (db; BKS.Cg-m+/+Lepr(db)/J), wildtype mice (dock7Lepr(db)+/+m) and laboratory BALB/c mice were examined. They were kept in single cages with access to laboratory chow with an 12/12 hour day/night circle. Lesions of the panniculus muscle (Ø 2 mm) were created in the center of the transparent window chamber and the subsequent muscular wound healing was then observed for a period of 22 days. Important analytic parameters included vessel diameter, red blood cell velocity, vascular permeability, and leakage of muscle capillaries and post capillary venules. The key parameters were functional capillary density (FCD) and angiogenesis positive area (APA). Results: We established a model which allows high resolution in vivo imaging of functional angiogenesis in diabetic wounds. As expected, db mice showed impaired wound closure (day 22) compared to wounds of BALB/c or WT mice (day 15). FCD was lower in diabetic mice compared to WT and BALB/c during the entire observation period. The dynamics of angiogenesis also decreased in db mice, as reflected by the lowest APA levels. Significant variations in the skin buildup were observed, with the greatest skin depth in db mice. Furthermore, in db mice, the dermis:subcutaneous ratio was highly shifted towards the subcutaneous layers as opposed to WT or BALB/c mice. Conclusion: Using this new in vivo model of the skinfold chamber, it was possible to analyze and quantify microangiopathical changes which are essential for a better understanding of the pathophysiology of disturbed wound healing. Research in microcirculation is important to display perfusion in wounds versus healthy tissue. Using our model, we were able to compare wound healing in diabetic and healthy mice. We were also able to objectively analyze perfusion in wound edges and compare microcirculatory parameters. This model may be well suited to augment different therapeutic options.
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spelling pubmed-47647942016-03-07 A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds Langer, Stefan Beescho, Christian Ring, Andrej Dorfmann, Olivia Steinau, Hans Ulrich Spindler, Nick GMS Interdiscip Plast Reconstr Surg DGPW Article Introduction: Diabetes mellitus describes a dysregulation of glucose metabolism due to improper insulin secretion, reduced insulin efficacy or both. It is a well-known fact that diabetic patients are likely to suffer from impaired wound healing, as diabetes strongly affects tissue angiogenesis. Until now, no satisfying in vivo murine model has been established to analyze the dynamics of angiogenesis during diabetic wound healing. To help understand the pathophysiology of diabetes and its effect on angiogenesis, a novel in vivo murine model was established using the skinfold chamber in mice. Materials and Methods: Mutant diabetic mice (db; BKS.Cg-m+/+Lepr(db)/J), wildtype mice (dock7Lepr(db)+/+m) and laboratory BALB/c mice were examined. They were kept in single cages with access to laboratory chow with an 12/12 hour day/night circle. Lesions of the panniculus muscle (Ø 2 mm) were created in the center of the transparent window chamber and the subsequent muscular wound healing was then observed for a period of 22 days. Important analytic parameters included vessel diameter, red blood cell velocity, vascular permeability, and leakage of muscle capillaries and post capillary venules. The key parameters were functional capillary density (FCD) and angiogenesis positive area (APA). Results: We established a model which allows high resolution in vivo imaging of functional angiogenesis in diabetic wounds. As expected, db mice showed impaired wound closure (day 22) compared to wounds of BALB/c or WT mice (day 15). FCD was lower in diabetic mice compared to WT and BALB/c during the entire observation period. The dynamics of angiogenesis also decreased in db mice, as reflected by the lowest APA levels. Significant variations in the skin buildup were observed, with the greatest skin depth in db mice. Furthermore, in db mice, the dermis:subcutaneous ratio was highly shifted towards the subcutaneous layers as opposed to WT or BALB/c mice. Conclusion: Using this new in vivo model of the skinfold chamber, it was possible to analyze and quantify microangiopathical changes which are essential for a better understanding of the pathophysiology of disturbed wound healing. Research in microcirculation is important to display perfusion in wounds versus healthy tissue. Using our model, we were able to compare wound healing in diabetic and healthy mice. We were also able to objectively analyze perfusion in wound edges and compare microcirculatory parameters. This model may be well suited to augment different therapeutic options. German Medical Science GMS Publishing House 2016-02-18 /pmc/articles/PMC4764794/ /pubmed/26955508 http://dx.doi.org/10.3205/iprs000088 Text en Copyright © 2016 Langer et al. http://creativecommons.org/licenses/by/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution 4.0 License.
spellingShingle Article
Langer, Stefan
Beescho, Christian
Ring, Andrej
Dorfmann, Olivia
Steinau, Hans Ulrich
Spindler, Nick
A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds
title A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds
title_full A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds
title_fullStr A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds
title_full_unstemmed A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds
title_short A new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds
title_sort new in vivo model using a dorsal skinfold chamber to investigate microcirculation and angiogenesis in diabetic wounds
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4764794/
https://www.ncbi.nlm.nih.gov/pubmed/26955508
http://dx.doi.org/10.3205/iprs000088
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