°”ÍűTV researchers make skin cells âcrawlâ together to heal wounds treated with unique hydrogel layer
Time may not heal all wounds, but a proprietary mix of peptides and gel developed by °”ÍűTV researchers heals most.
A team led by Faculty of Applied Science & Engineering Professor Milica Radisic has demonstrated for the first time that a peptide-hydrogel biomaterial prompts skin cells to âcrawlâ toward one another, closing chronic, non-healing wounds often associated with diabetes such as bed sores and foot ulcers.
The team tested their biomaterial on healthy cells from the surface of human skin called keratinocytes as well as on keratinocytes derived from elderly diabetic patients. They saw non-healing wounds close 200 per cent faster than with no treatment and 60 per cent faster than treatment with a leading commercially used collagen-based product.
âWe were happy when we saw the cells crawl together much faster with our biomatieral, but if it didnât work with diabetic cells, that would have been the end of the story,â says Radisic. âBut even the diabetic cells travelled much faster â thatâs huge.â
Until now, most treatments for chronic wounds involved applying topical ointments that promote the growth of blood vessels to the area. But in diabetic patients, blood vessel growth is inhibited, making those treatments ineffective. Radisic and her team have been working with their special peptide â called QHREDGS or Q-peptide for short â for almost 10 years. They knew it promoted survival of many different cell types, including stem cells, heart cells and fibroblasts (the cells that make connective tissues) but had never applied it to wound healing.
âWe thought that if we were able to use our peptide to both promote survival and give these skin cells a substrate so they could crawl together, they would be able to close the wound more quickly,â says Radisic. âThat was the underlying hypothesis.â
At left, skin cells without the research teamâs peptide-hydrogel treatment. In the middle, cells treated with a low dose. At right, cells treated with a high dose. Skin cells migrate together fastest with a high dose of the peptide-hydrogel material (photo courtesy of Radisic Lab)
Radisic and PhD students Yun Xiao and Lewis Reis compared the Q-peptide-hydrogel mix to the commercially available collagen dressing, to hydrogels without the peptide and to no treatment. They found that a single dose of their peptide-hydrogel biomaterial closed the wounds in less than two weeks. Their work was published in the journal .
âCurrently, there are therapies for diabetic foot ulcers, but they can be improved,â says Xiao, the paperâs lead author. âDiabetic wound healing is a complicated condition, because many aspects of the normal wound healing process are disrupted â I know people with diabetic foot ulcers, and the possibility to improve their lives drove me throughout this work.â
The multidisciplinary team worked with Covalon Technologies Ltd., a company dedicated to the research and development and commercialization of novel health-care technologies, on this project. Covalonâs chief scientific officer, Val DiTizio, has been leading the partnership with Radisicâs group for about three years, and contributed its collagen-based wound-healing dressing, ColActive, as one of the controls.
âWe believe strongly in keeping abreast of new technologies being developed in academia,â says DiTizio, who is also working with Radisic on a bone-regeneration project. âCollaborations such as this one inform our future research directions and help make our products better.â
This finding could have big implications for many types of wound treatments, from recovery after a heart attack to healing post-surgery. Accelerated healing times also introduces the added benefit of reducing the opportunity for infection, says Reis.
âOne of the biggest challenges with the work was convincing our peers that the results we were getting were indeed true as they were staggering, even to us,â he says. âBeing confident in our methods and diligent in our research and analysis prevailed in the end.â