4.8 Article

Use of a fibrin-based system for enhancing angiogenesis and modulating inflammation in the treatment of hyperglycemic wounds

Journal

BIOMATERIALS
Volume 35, Issue 6, Pages 2001-2010

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2013.11.003

Keywords

Gene therapy; Diabetes; Wound healing; Angiogenesis; Inflammation; Keratinocyte

Funding

  1. Research Frontier Project, Science Foundation Ireland [06/RFP/ENM005]
  2. Science Foundation Ireland (SFI) [06/RFP/ENM005] Funding Source: Science Foundation Ireland (SFI)

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The complex pathophysiology of chronic ulceration in diabetic patients is poorly understood; diabetes-related lower limb amputation is a major health issue, which has limited effective treatment regimes in the clinic. This study attempted to understand the complex pathology of hyperglycemic wound healing by showing profound changes in gene expression profiles in wounded human keratinocytes in hyperglycemic conditions compared to normal glucose conditions. In the hyper-secretory wound microenvironment of hyperglycemia, Rab18, a secretory control molecule, was found to be significantly downregulated. Using a biomaterial platform for dual therapy targeting the two distinct pathways, this study aimed to resolve the major dysregulated pathways in hyperglycemic wound healing. To complement Rab18, and promote angiogenesis eNOS was also targeted, and this novel Rab18-eNOS therapy via a dynamically controlled 'fibrin-in-fibrin' delivery system, demonstrated enhanced wound closure, by increasing functional angiogenesis and reducing inflammation, in an alloxan-induced hyperglycemic preclinical ear ulcer model of compromised wound healing. (C) 2013 Elsevier Ltd. All rights reserved.

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