Literature DB >> 12891006

CD34+ blood cells accelerate vascularization and healing of diabetic mouse skin wounds.

E Sivan-Loukianova1, O A Awad, V Stepanovic, J Bickenbach, G C Schatteman.   

Abstract

Diabetes is characterized by poor circulation and impaired angiogenesis, which appear to contribute to the frequent skin lesions and poor wound healing common in diabetic patients. Therapies to improve circulation commonly improve wound healing in diabetic patients. Administration of circulating CD34+ cells, cells that can function as endothelial cell progenitors, accelerates blood flow restoration to ischemic limbs of diabetic mice. We have investigated the potential of these cells to accelerate revascularization and healing in full-thickness skin wounds of hypoinsulinemic (streptozotocin-treated) diabetic mice. Wounds were injected with human CD34+ or CD34- peripheral blood mononuclear cells or no cells, and analyzed for vascularity and healing at various times thereafter. Treatment with CD34+ enriched cells decreased wound size by 4 days after treatment, accelerated epidermal healing, and rapidly and dramatically accelerated revascularization of the wounds compared to controls. Initially increased vascularization was mediated principally by an increase in vessel diameter, but later, both an increase in vascular size and number were observed. These findings indicate that blood-derived progenitors may have therapeutic potential in the treatment of skin lesions in the setting of diabetes, and give insights into how bone marrow cells exert their effects on neovascularization. Copyright 2003 S. Karger AG, Basel

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Year:  2003        PMID: 12891006     DOI: 10.1159/000072701

Source DB:  PubMed          Journal:  J Vasc Res        ISSN: 1018-1172            Impact factor:   1.934


  61 in total

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Review 9.  Recent advances in bone regeneration using adult stem cells.

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10.  HOXA3 modulates injury-induced mobilization and recruitment of bone marrow-derived cells.

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