Adipose-Derived Stromal Cells Seeded in Pullulan-Collagen Hydrogels Improve Healing in Murine Burns

伤口愈合 自愈水凝胶 医学 脂肪组织 间充质干细胞 普鲁兰 化学 促炎细胞因子 疤痕 干细胞 皮肤修复 血管生成 细胞疗法 细胞生物学 病理 外科 炎症 免疫学 癌症研究 内科学 生物 有机化学 多糖 生物化学
作者
Janos A. Barrera,Artem A. Trotsyuk,Zeshaan N. Maan,Clark A. Bonham,Madelyn R. Larson,Paul A. Mittermiller,Dominic Henn,Kellen Chen,Chyna J. Mays,Smiti Mittal,Alana M. Mermin-Bunnell,Dharshan Sivaraj,Serena L. Jing,Mélanie Rodrigues,Sun Hyung Kwon,Chikage Noishiki,Jagannath Padmanabhan,Yuanwen Jiang,Simiao Niu,Mohammed Inayathullah,Jayakumar Rajadas,Michael Januszyk,Geoffrey C. Gurtner
出处
期刊:Tissue Engineering Part A [Mary Ann Liebert]
卷期号:27 (11-12): 844-856 被引量:41
标识
DOI:10.1089/ten.tea.2020.0320
摘要

Burn scars and scar contractures cause significant morbidity for patients. Recently, cell-based therapies have been proposed as an option for improving healing and reducing scarring after burn injury, through their known proangiogenic and immunomodulatory paracrine effects. Our laboratory has developed a pullulan-collagen hydrogel that, when seeded with mesenchymal stem cells (MSCs), improves cell viability and augments their proangiogenic capacity in vivo. Concurrently, recent research suggests that prospective isolation of cell subpopulations with desirable transcriptional profiles can be used to further improve cell-based therapies. In this study, we examined whether adipose-derived stem cell (ASC)-seeded hydrogels could improve wound healing following thermal injury using a murine contact burn model. Partial thickness contact burns were created on the dorsum of mice. On days 5 and 10 following injury, burns were debrided and received either ASC hydrogel, ASC injection alone, hydrogel alone, or no treatment. On days 10 and 25, burns were harvested for histologic and molecular analysis. This experiment was repeated using CD26+/CD55+ FACS-enriched ASCs to further evaluate the regenerative potential of ASCs in wound healing. ASC hydrogel-treated burns demonstrated accelerated time to reepithelialization, greater vascularity, and increased expression of the proangiogenic genes MCP-1, VEGF, and SDF-1 at both the mRNA and protein level. Expression of the profibrotic gene Timp1 and proinflammatory gene Tnfa was downregulated in ASC hydrogel-treated burns. ASC hydrogel-treated burns exhibited reduced scar area compared to hydrogel-treated and control wounds, with equivalent scar density. CD26+/CD55+ ASC hydrogel treatment resulted in accelerated healing, increased dermal appendage count, and improved scar quality with a more reticular collagen pattern. Here we find that ASC hydrogel therapy is effective for treating burns, with demonstrated proangiogenic, fibromodulatory, and immunomodulatory effects. Enrichment for CD26+/CD55+ ASCs has additive benefits for tissue architecture and collagen remodeling postburn injury. Research is ongoing to further facilitate clinical translation of this promising therapeutic approach. Burns remain a significant public health burden. Stem cell therapy has gained attention as a promising approach for treating burns. We have developed a pullulan-collagen biomimetic hydrogel scaffold that can be seeded with adipose-derived stem cells (ASCs). We assessed the delivery and activity of our scaffold in a murine contact burn model. Our results suggest that localized delivery of ASC hydrogel treatment is a promising approach for the treatment of burn wounds, with the potential for rapid clinical translation. We believe our work will have broad implications for both hydrogel therapeutics and regenerative medicine and will be of interest to the general scientific community.
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