Application of an instructive hydrogel accelerates re-epithelialization of xenografted human skin wounds

伤口愈合 角质形成细胞 人体皮肤 自愈水凝胶 表皮(动物学) 医学 伤口闭合 体外 癌症研究 化学 外科 生物 解剖 生物化学 遗传学 有机化学
作者
Holly D. Sparks,Serena Mandla,Katrina Vizely,Nicole L. Rosin,Milica Radisic,Jeff Biernaskie
出处
期刊:Scientific Reports [Nature Portfolio]
卷期号:12 (1)
标识
DOI:10.1038/s41598-022-18204-w
摘要

Abstract Poor quality (eg. excessive scarring) or delayed closure of skin wounds can have profound physical and pyschosocial effects on patients as well as pose an enormous economic burden on the healthcare system. An effective means of improving both the rate and quality of wound healing is needed for all patients suffering from skin injury. Despite wound care being a multi-billion-dollar industry, effective treatments aimed at rapidly restoring the skin barrier function or mitigating the severity of fibrotic scar remain elusive. Previously, a hydrogel conjugated angiopoietin-1 derived peptide (QHREDGS; Q-peptide) was shown to increase keratinocyte migration and improve wound healing in diabetic mice. Here, we evaluated the effect of this Q-Peptide Hydrogel on human skin wound healing using a mouse xenograft model. First, we confirmed that the Q-Peptide Hydrogel promoted the migration of adult human keratinocytes and modulated their cytokine profile in vitro. Next, utilizing our human to mouse split-thickness skin xenograft model, we found improved healing of wounded human epidermis following Q-Peptide Hydrogel treatment. Importantly, Q-Peptide Hydrogel treatment enhanced this wound re-epithelialization via increased keratinocyte migration and survival, rather than a sustained increase in proliferation. Overall, these data provide strong evidence that topical application of QHREDGS peptide-modified hydrogels results in accelerated wound closure that may lead to improved outcomes for patients.

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