Literature DB >> 19903305

Stimulated neovascularization, inflammation resolution and collagen maturation in healing rat cutaneous wounds by a heparan sulfate glycosaminoglycan mimetic, OTR4120.

Miao Tong1, Bastiaan Tuk, Ineke M Hekking, Marcel Vermeij, Denis Barritault, Johan W van Neck.   

Abstract

Heparan sulfate glycosaminoglycans (HS-GAGs) are not only the structural elements of tissue architecture but also regulate the bioavailability and transduction pathways of heparan sulfate-bound polypeptides released by cells or the extracellular matrix. Heparan sulfate-bound polypeptides include inflammatory mediators, chemokines, angiogenic factors, morphogens, and growth-promoting factors that induce cell migration, proliferation, and differentiation in wound healing. OTR4120, a polymer engineered to mimic the properties of HS-GAGs, is used to replace the natural HS-GAGs that are degraded during wound repair, and enhance the tissue regeneration by preserving the cellular microenvironment and the endogenous signals needed for tissue regeneration. We previously demonstrated that OTR4120 treatment had a long-term effect on increasing breaking strength and vasodilation in healing rat full-thickness excisional wounds. The present study investigates the underlying mechanisms of the effects of OTR4120 treatment in improving the quality of cutaneous wound repair. We found that OTR4120 treatment stimulated inflammation resolution and increased neovascularization. OTR4120 treatment also promoted epidermal migration and proliferation during reepithelialization. Moreover, the granulation tissue formation and collagen maturation were improved in OTR4120-treated wounds. Three months after wounding, the effects of OTR4120 treatment on vascularization and inflammation resolution were normalized, except for an improved neodermis. We conclude that OTR4120 is a potential matrix therapeutic agent that ensures the quality of normal cutaneous wound repair and may restore impaired wound healing characterized by deficient angiogenesis and prolonged inflammation.

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Year:  2009        PMID: 19903305     DOI: 10.1111/j.1524-475X.2009.00548.x

Source DB:  PubMed          Journal:  Wound Repair Regen        ISSN: 1067-1927            Impact factor:   3.617


  20 in total

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3.  Specific effects of fibrinogen and the γA and γ'-chain fibrinogen variants on angiogenesis and wound healing.

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Journal:  Tissue Eng Part A       Date:  2014-08-05       Impact factor: 3.845

4.  Refractory sickle cell leg ulcer: is heparan sulphate a new hope?

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5.  The Biomechanical Effects of Resuscitation Colloids on the Compromised Lung Endothelial Glycocalyx.

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6.  Diabetes-impaired wound healing is improved by matrix therapy with heparan sulfate glycosaminoglycan mimetic OTR4120 in rats.

Authors:  Miao Tong; Bastiaan Tuk; Peng Shang; Ineke M Hekking; Esther M G Fijneman; Marnix Guijt; Steven E R Hovius; Johan W van Neck
Journal:  Diabetes       Date:  2012-06-20       Impact factor: 9.461

7.  TAT-Mediated Acidic Fibroblast Growth Factor Delivery to the Dermis Improves Wound Healing of Deep Skin Tissue in Rat.

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Review 8.  Future Prospects for Scaffolding Methods and Biomaterials in Skin Tissue Engineering: A Review.

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9.  A Rapid Response to Matrix Therapy With RGTA in Severe Epidermolysis Bullosa.

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10.  Glycosaminoglycan content of a mineralized collagen scaffold promotes mesenchymal stem cell secretion of factors to modulate angiogenesis and monocyte differentiation.

Authors:  Marley J Dewey; Vasiliki Kolliopoulos; Mai T Ngo; Brendan A C Harley
Journal:  Materialia (Oxf)       Date:  2021-06-18
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