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Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing

The lack of vascularization associated with deep burns delays the construction of wound beds, increases the risks of infection, and leads to the formation of hypertrophic scars or disfigurement. To address this challenge, we have fabricated a multi-functional pro-angiogenic molecule by grafting inte...

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Autores principales: Song, Hengyue, Gao, Kewa, Hao, Dake, Li, Andrew, Liu, Ruiwu, Anggito, Bryan, Yin, Boyan, Jin, Qianyu, Dartora, Vanessa, Lam, Kit S., Smith, Lucas R., Panitch, Alyssa, Zhou, Jianda, Farmer, Diana L., Wang, Aijun
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10014525/
https://www.ncbi.nlm.nih.gov/pubmed/36937891
http://dx.doi.org/10.3389/fphar.2023.1125209
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author Song, Hengyue
Gao, Kewa
Hao, Dake
Li, Andrew
Liu, Ruiwu
Anggito, Bryan
Yin, Boyan
Jin, Qianyu
Dartora, Vanessa
Lam, Kit S.
Smith, Lucas R.
Panitch, Alyssa
Zhou, Jianda
Farmer, Diana L.
Wang, Aijun
author_facet Song, Hengyue
Gao, Kewa
Hao, Dake
Li, Andrew
Liu, Ruiwu
Anggito, Bryan
Yin, Boyan
Jin, Qianyu
Dartora, Vanessa
Lam, Kit S.
Smith, Lucas R.
Panitch, Alyssa
Zhou, Jianda
Farmer, Diana L.
Wang, Aijun
author_sort Song, Hengyue
collection PubMed
description The lack of vascularization associated with deep burns delays the construction of wound beds, increases the risks of infection, and leads to the formation of hypertrophic scars or disfigurement. To address this challenge, we have fabricated a multi-functional pro-angiogenic molecule by grafting integrin αvβ3 ligand LXW7 and collagen-binding peptide (SILY) to a dermatan sulfate (DS) glycosaminoglycan backbone, named LXW7-DS-SILY (LDS), and further employed this to functionalize collagen-based Integra scaffolds. Using a large deep burn wound model in C57/BLK6 mice (8–10 weeks old, 26–32g, n = 39), we demonstrated that LDS-modified collagen-based Integra scaffolds loaded with endothelial cells (ECs) accelerate wound healing rate, re-epithelialization, vascularization, and collagen deposition. Specifically, a 2 cm × 3 cm full-thickness skin burn wound was created 48 h after the burn, and then wounds were treated with four groups of different dressing scaffolds, including Integra + ECs, Integra + LDS, and Integra + LDS + ECs with Integra-only as the control. Digital photos were taken for wound healing measurement on post-treatment days 1, 7, 14, 21, 28, and 35. Post-treatment photos revealed that treatment with the Intgera + LDS + ECs scaffold exhibited a higher wound healing rate in the proliferation phase. Histology results showed significantly increased re-epithelialization, increased collagen deposition, increased thin and mixed collagen fiber content, increased angiogenesis, and shorter wound length within the Integra + LDS + ECs group at Day 35. On Day 14, the Integra + LDS + ECs group showed the same trend. The relative proportions of collagen changed from Day 14 to Day 35 in the Integra + LDS + ECs and Integra + ECs groups demonstrated decreased thick collagen fiber deposition and greater thin and mixed collagen fiber deposition. LDS-modified Integra scaffolds represent a promising novel treatment to accelerate deep burn wound healing, thereby potentially reducing the morbidity associated with open burn wounds. These scaffolds can also potentially reduce the need for autografting and morbidity in patients with already limited areas of harvestable skin.
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spelling pubmed-100145252023-03-16 Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing Song, Hengyue Gao, Kewa Hao, Dake Li, Andrew Liu, Ruiwu Anggito, Bryan Yin, Boyan Jin, Qianyu Dartora, Vanessa Lam, Kit S. Smith, Lucas R. Panitch, Alyssa Zhou, Jianda Farmer, Diana L. Wang, Aijun Front Pharmacol Pharmacology The lack of vascularization associated with deep burns delays the construction of wound beds, increases the risks of infection, and leads to the formation of hypertrophic scars or disfigurement. To address this challenge, we have fabricated a multi-functional pro-angiogenic molecule by grafting integrin αvβ3 ligand LXW7 and collagen-binding peptide (SILY) to a dermatan sulfate (DS) glycosaminoglycan backbone, named LXW7-DS-SILY (LDS), and further employed this to functionalize collagen-based Integra scaffolds. Using a large deep burn wound model in C57/BLK6 mice (8–10 weeks old, 26–32g, n = 39), we demonstrated that LDS-modified collagen-based Integra scaffolds loaded with endothelial cells (ECs) accelerate wound healing rate, re-epithelialization, vascularization, and collagen deposition. Specifically, a 2 cm × 3 cm full-thickness skin burn wound was created 48 h after the burn, and then wounds were treated with four groups of different dressing scaffolds, including Integra + ECs, Integra + LDS, and Integra + LDS + ECs with Integra-only as the control. Digital photos were taken for wound healing measurement on post-treatment days 1, 7, 14, 21, 28, and 35. Post-treatment photos revealed that treatment with the Intgera + LDS + ECs scaffold exhibited a higher wound healing rate in the proliferation phase. Histology results showed significantly increased re-epithelialization, increased collagen deposition, increased thin and mixed collagen fiber content, increased angiogenesis, and shorter wound length within the Integra + LDS + ECs group at Day 35. On Day 14, the Integra + LDS + ECs group showed the same trend. The relative proportions of collagen changed from Day 14 to Day 35 in the Integra + LDS + ECs and Integra + ECs groups demonstrated decreased thick collagen fiber deposition and greater thin and mixed collagen fiber deposition. LDS-modified Integra scaffolds represent a promising novel treatment to accelerate deep burn wound healing, thereby potentially reducing the morbidity associated with open burn wounds. These scaffolds can also potentially reduce the need for autografting and morbidity in patients with already limited areas of harvestable skin. Frontiers Media S.A. 2023-03-01 /pmc/articles/PMC10014525/ /pubmed/36937891 http://dx.doi.org/10.3389/fphar.2023.1125209 Text en Copyright © 2023 Song, Gao, Hao, Li, Liu, Anggito, Yin, Jin, Dartora, Lam, Smith, Panitch, Zhou, Farmer and Wang. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pharmacology
Song, Hengyue
Gao, Kewa
Hao, Dake
Li, Andrew
Liu, Ruiwu
Anggito, Bryan
Yin, Boyan
Jin, Qianyu
Dartora, Vanessa
Lam, Kit S.
Smith, Lucas R.
Panitch, Alyssa
Zhou, Jianda
Farmer, Diana L.
Wang, Aijun
Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing
title Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing
title_full Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing
title_fullStr Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing
title_full_unstemmed Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing
title_short Engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing
title_sort engineered multi-functional, pro-angiogenic collagen-based scaffolds loaded with endothelial cells promote large deep burn wound healing
topic Pharmacology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10014525/
https://www.ncbi.nlm.nih.gov/pubmed/36937891
http://dx.doi.org/10.3389/fphar.2023.1125209
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