Enhancing Diabetic Wound Healing Through Improved Angiogenesis: The Role of Emulsion‐Based Core‐Shell Micro/Nanofibrous Scaffold with Sustained CuO Nanoparticle Delivery

Author:

Alizadeh Sanaz12ORCID,Samadikuchaksaraei Ali3ORCID,Jafari Davod3,Orive Gorka4567,Dolatshahi‐Pirouz Alireza8ORCID,Pezeshki‐Modaress Mohamad91011ORCID,Gholipourmalekabadi Mazaher12312ORCID

Affiliation:

1. Cellular and Molecular Research Center Iran University of Medical Sciences Tehran 1449614535 Iran

2. Department of Tissue Engineering & Regenerative Medicine Faculty of Advanced Technologies in Medicine Iran University of Medical Sciences Tehran Iran

3. Department of Medical Biotechnology Faculty of Allied Medicine Iran University of Medical Sciences Tehran 1449614535 Iran

4. NanoBioCel Group Laboratory of Pharmaceutics School of Pharmacy University of the Basque Country UPV/EHU Paseo de la Universidad 7 Vitoria‐Gasteiz 01006 Spain

5. Biomedical Research Networking Centre in Bioengineering Biomaterials and Nanomedicine (CIBER‐BBN) Vitoria‐Gasteiz 01006 Spain

6. University Institute for Regenerative Medicine and Oral Implantology – UIRMI (UPV/EHU‐Fundación Eduardo Anitua) Vitoria 01006 Spain

7. Bioaraba NanoBioCel Research Group Vitoria‐Gasteiz 01006 Spain

8. Department of Health Technology Technical University of Denmark Lyngby 2800 Denmark

9. Burn Research Center Iran University of Medical Sciences Tehran 1449614535 Iran

10. Department of Plastic and Reconstructive Surgery Hazrat Fatemeh Hospital School of Medicine Iran University of Medical Sciences Tehran 1449614535 Iran

11. Stem Cell and Regenerative Medicine Research Center Iran University of Medical Sciences Tehran 1449614535 Iran

12. NanoBiotechnology & Regenerative Medicine Innovation Group Noavarn Salamat ZHINO (PHC) Tehran 1949635882 Iran

Abstract

AbstractAttempts are made to design a system for sustaining the delivery of copper ions into diabetic wounds and induce angiogenesis with minimal dose‐dependent cytotoxicity. Here, a dual drug‐delivery micro/nanofibrous core‐shell system is engineered using polycaprolactone/sodium sulfated alginate‐polyvinyl alcohol (PCL/SSA‐PVA), as core/shell parts, by emulsion electrospinning technique to optimize sustained delivery of copper oxide nanoparticles (CuO NP). Herein, different concentrations of CuO NP (0.2, 0.4, 0.8, and 1.6%w/w) are loaded into the core part of the core‐shell system. The morphological, biomechanical, and biocompatibility properties of the scaffolds are fully determined in vitro and in vivo. The 0.8%w/w CuO NP scaffold reveals the highest level of tube formation in HUVEC cells and also upregulates the pro‐angiogenesis genes (VEGFA and bFGF) expression with no cytotoxicity effects. The presence of SSA and its interaction with CuO NP, and also core‐shell structure sustain the release of the nanoparticles and provide a non‐toxic microenvironment for cell adhesion and tube formation, with no sign of adverse immune response in vivo. The optimized scaffold significantly accelerates diabetic wound healing in a rat model. This study strongly suggests the 0.8%w/w CuO NP‐loaded PCL/SSA‐PVA as an excellent diabetic wound dressing with significantly improved angiogenesis and wound healing.

Funder

Iran University of Medical Sciences

Publisher

Wiley

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