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      ISOLATION OF CD248-EXPRESSING STROMAL VASCULAR FRACTION FOR TARGETED IMPROVEMENT OF WOUND HEALING

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          Abstract

          Wound healing remains a global issue of disability, cost, and health. Addition of cells from the stromal vascular fraction of adipose tissue has been shown to increase the rate of full thickness wound closure. The present study aimed to investigate the angiogenic mechanisms of CD248+ stromal vascular fraction (SVF) cells in the context of full thickness excisional wounds. Single cell transcriptional analysis was used to identify and cluster angiogenic gene-expressing cells, which was then correlated with surface marker expression. SVF cells isolated from human lipoaspirate were FACS sorted based on the presence of CD248. Cells were analyzed for angiogenic gene expression and ability to promote microvascular tubule formation in vitro. Following this, 6mm full thickness dermal wounds were created on the dorsa of immunocompromised mice and then treated with CD248+, CD248−, or unsorted SVF cells delivered in a pullalan-collagen hydrogel or the hydrogel alone. Wounds were measured every other day photometrically until closure. Wounds were also evaluated histologically at 7 and 14 days post-wounding and when fully healed to assess for re-epithelialization and development of neovasculature. Wounds treated with CD248+ cells healed significantly faster than other treatment groups, and at 7 days, had quantitatively more re-epithelialization. Concurrently, immunohistochemistry of CD31 revealed a much higher presence of vascularity in the CD248+ SVF cells treated group at the time of healing and at 14 days post-op, consistent with a pro-angiogenic effect of CD248+ cells in vivo. Therefore, using CD248+ pro-angiogenic cells obtained from SVF presents a viable strategy in wound healing by promoting increased vessel growth in the wound.

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          Author and article information

          Journal
          9310939
          21119
          Wound Repair Regen
          Wound Repair Regen
          Wound repair and regeneration : official publication of the Wound Healing Society [and] the European Tissue Repair Society
          1067-1927
          1524-475X
          19 May 2017
          18 May 2017
          May 2017
          18 May 2018
          : 25
          : 3
          : 414-422
          Affiliations
          [1 ]Hagey Laboratory for Pediatric Regenerative Medicine, Department of Surgery, Division of Plastic Surgery, Stanford University School of Medicine, Stanford, California, USA
          [2 ]Institute for Stem Cell Biology and Regenerative Medicine, Stanford University School of Medicine, Stanford, California, USA
          Author notes
          [* ]Correspondence: Derrick C. Wan, MD, Associate Professor of Surgery, Stanford University Medical Center, Stanford University School of Medicine, 257 Campus Drive, Stanford, CA 94305, Tel 650-736-2776, dwan@ 123456stanford.edu
          Article
          PMC5568953 PMC5568953 5568953 nihpa876587
          10.1111/wrr.12542
          5568953
          28464475
          50c7f0fa-830a-4fa5-84ef-0f67f7f26a4d
          History
          Categories
          Article

          wound healing,angiogenesis,CD248,full thickness dermal wounds

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