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Abstract
Introduction Investigators have struggled to produce a reliable chronic wound model. Recent progress with antioxidant enzyme inhibitors shows promise, but mortality rates are high. We modified the dosage and administration of an antioxidant enzyme inhibitor regimen to reduce mortality while inducing a chronic wound environment.
Research design and methods To chemically induce a chronic wound environment, we applied modified doses of catalase (3-amino-1,2,4-triazole; intraperitoneal 0.5 g/kg) and glutathione peroxidase (mercaptosuccinic acid; topical 300 mg/kg) inhibitors to the dorsal wounds of 11-week-old db/db mice. A cohort of these mice was treated with a collagen-glycosaminoglycan scaffold. Both groups were compared with Diabetic control mice.
Results This study successfully induced a chronic wound in 11-week-old db/db mice, with no animal deaths. The antioxidant enzyme treated groups showed delayed wound contraction and significantly higher levels of inflammatory tissue, collagen deposition, cellular proliferation and leukocyte infiltration than the Diabetic control group. Angiogenesis was significantly higher in the antioxidant enzyme treated groups, but the vessels were immature and friable. Scaffold engraftment was poor but appeared to promote blood vessel maturation.
Conclusions Overall, the two in vivo groups treated with the antioxidant enzyme inhibitors appeared to be arrested in the inflammatory stage of wound healing, while the Diabetic control group progressed to the maturation phase and ultimately remodeling. This model may be instrumental for the development of new wound therapeutics.
- chronic wound(s)
- mouse model(s)
- regeneration
- wound healing
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Footnotes
Contributors ACP and DPO conceived and designed the experiment. ACP, BM, and YA performed the animal experiments. ACP and VH analyzed the animal data. YE, MK, PS, and SF performed the staining and histology analysis. VH performed the statistical analysis. ACP wrote the paper. VH, MK, YE, and DPO edited the manuscript. The manuscript was reviewed by all authors. ACP is the guarantor of this work and, as such, had full access to all the data in the study and takes responsibility for the integrity of the data and the accuracy of the data analysis.
Funding This project was supported through grants to Brigham and Women’s Hospital from Integra LifeSciences, Inc., and The Stepping Strong Foundation.
Competing interests DPO receives grant support through a sponsored research agreement through Integra Lifesciences. DPO is a consultant for Integra Lifesciences.
Patient consent for publication Not required.
Provenance and peer review Not commissioned; internally peer reviewed.
Data availability statement Data are available on reasonable written request.