Abstract

Injury-responsive coding genes are recognized as a major cornerstone in wound healing. As much as 97% of human DNA does not encode for protein and has been called junk. microRNAs (miRs) represent a class of non-coding (nc) genes that can not only be no longer regarded as junk but they represent a key regulatory mechanism that control the functionality of large sets of coding target genes. miRs themselves do not encode protein but the function of one-third of the coding human genome is regulated by miRs. miRs are evolutionarily conserved, approximately 22-nucleotide single-stranded RNAs that post-transcriptionally silences genes by inducing mRNA degradation or by inhibiting translation. Thus, miR biology connects mRNA to their biological function. Yet, information on the significance of miRs in wound healing is scanty. In 2008, our group reported the first work on how miRs may regulate wound angiogenesis and has since then actively published in the field of miRs and wound healing. This proposal builds on our recent published observation that wound-responsive repression of cutaneous miR-200b turns on wound angiogenesis which is de-regulated during diabetes mellitus. Endothelial cells of patients with adult onset (type-2) diabetes feature elevated miR-200b. Consistent findings were noted in diabetic mice. These data lead us to question the mechanism of how miR-200b accumulates in the setting of diabetic wounds (AIM1) and how the resultant miR-200b-dependent downstream pathways mitigate wound angiogenesis (AIMS 2&3). The following 3 aims are proposed:
AIM 1 Investigate the molecular mechanisms causing aberrant induction of endothelial miR-200b in diabetic wounds. 1.1 Loss of GATA2 induces endothelial miR-200b expression; 1.2 Diabetic wound-associated p53 activation supports endothelial miR-200b expression.
AIM 2 Determine the significance of elevated endothelial miR-200b in disruption of VEGF signaling. 2.1 Aberrant induction of endothelial miR-200b blocks VEGF expression in diabetic wounds. 2.2 Loss of diabetic wound-site endothelial VEGFR1 is caused by high miR-200b. 2.3 miR-200b silences diabetic wound-site CAGE and impairs VEGF signaling.
AIM 3 Establish the molecular mechanisms underlying dysregulated miR-200b in impairing endothelial cell turnover and impaired angiogenesis in diabetic wounds. 3.1 miR-200b-ZEB1 signaling enhances endothelial apoptosis in diabetic wound-edge. 3.2 High endothelial miR-200b in diabetic wound-edge tissue drives endothelial apoptosis via a Bcl-2 dependent mechanism. 3.3 miR-200b silences CXCL1 and IL-8 and impairs endothelial cell proliferation in diabetic wounds causing impaired angiogenesis.

Public Health Relevance

In the United States, skin wounds affect 6.5 million patients placing a major burden, estimated at US $25 billion annually, on society. Poor vascular supply of the wound tissue is a major contributor to wound chronicity specifically in diabetic ulcers. The proposed project aims address a novel regulatory mechanism (microRNA) that simultaneously governs multiple pathways related to vascularization of the wound tissue. Specifically, the proposal focuses on microRNA200b as a key regulator of wound perfusion.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM108014-03
Application #
9195141
Study Section
Surgery, Anesthesiology and Trauma Study Section (SAT)
Program Officer
Somers, Scott D
Project Start
2015-01-01
Project End
2018-12-31
Budget Start
2017-01-01
Budget End
2017-12-31
Support Year
3
Fiscal Year
2017
Total Cost
$263,340
Indirect Cost
$92,340

  Institution

Name
Ohio State University
Department
Surgery
Type
Schools of Medicine
DUNS #
832127323
City
Columbus
State
OH
Country
United States
Zip Code
43210

  Publications

Das Ghatak, Piya; Mathew-Steiner, Shomita S; Pandey, Priyanka et al. (2018) A surfactant polymer dressing potentiates antimicrobial efficacy in biofilm disruption. Sci Rep 8:873
Sinha, Mithun; Sen, Chandan K; Singh, Kanhaiya et al. (2018) Direct conversion of injury-site myeloid cells to fibroblast-like cells of granulation tissue. Nat Commun 9:936
Das, Amitava; Datta, Soma; Roche, Eric et al. (2018) Novel mechanisms of Collagenase Santyl Ointment (CSO) in wound macrophage polarization and resolution of wound inflammation. Sci Rep 8:1696
Gnyawali, Surya C; Blum, Kevin; Pal, Durba et al. (2017) Retooling Laser Speckle Contrast Analysis Algorithm to Enhance Non-Invasive High Resolution Laser Speckle Functional Imaging of Cutaneous Microcirculation. Sci Rep 7:41048
Singh, Kanhaiya; Pal, Durba; Sinha, Mithun et al. (2017) Epigenetic Modification of MicroRNA-200b Contributes to Diabetic Vasculopathy. Mol Ther 25:2689-2704
Gallego-Perez, Daniel; Pal, Durba; Ghatak, Subhadip et al. (2017) Topical tissue nano-transfection mediates non-viral stroma reprogramming and rescue. Nat Nanotechnol 12:974-979
Roy, Sashwati (2016) miRNA in Macrophage Development and Function. Antioxid Redox Signal 25:795-804
Gordillo, Gayle M; Biswas, Ayan; Khanna, Savita et al. (2016) Multidrug resistance-associated protein-1 (MRP-1)-dependent glutathione disulfide (GSSG) efflux as a critical survival factor for oxidant-enriched tumorigenic endothelial cells. J Biol Chem 291:14394
Sen, Chandan K; Ghatak, Subhadip; Gnyawali, Surya C et al. (2016) Cutaneous Imaging Technologies in Acute Burn and Chronic Wound Care. Plast Reconstr Surg 138:119S-28S
Ghatak, Subhadip; Li, Jilong; Chan, Yuk C et al. (2016) AntihypoxamiR functionalized gramicidin lipid nanoparticles rescue against ischemic memory improving cutaneous wound healing. Nanomedicine 12:1827-1831

Showing the most recent 10 out of 22 publications