Dual scaffold delivery of miR-210 mimic and miR-16 inhibitor enhances angiogenesis and osteogenesis to accelerate bone healing

Irene Mencía Castaño; Rosanne M Raftery; Gang Chen; Brenton Cavanagh; Brian Quinn; Garry P Duffy; Caroline M Curtin; Fergal J O'Brien

doi:10.1016/j.actbio.2023.09.049

Dual scaffold delivery of miR-210 mimic and miR-16 inhibitor enhances angiogenesis and osteogenesis to accelerate bone healing

Acta Biomater. 2023 Dec:172:480-493. doi: 10.1016/j.actbio.2023.09.049. Epub 2023 Oct 4.

Authors

Irene Mencía Castaño¹, Rosanne M Raftery², Gang Chen³, Brenton Cavanagh⁴, Brian Quinn¹, Garry P Duffy⁵, Caroline M Curtin⁶, Fergal J O'Brien⁷

Affiliations

¹ Tissue Engineering Research Group, Department of Anatomy, Royal College of Surgeons in Ireland (RCSI), 123 St. Stephens Green, Dublin 2, Ireland.
² Tissue Engineering Research Group, Department of Anatomy, Royal College of Surgeons in Ireland (RCSI), 123 St. Stephens Green, Dublin 2, Ireland; School of Pharmacy, RCSI, Dublin, Ireland.
³ Department of Physiology and Medical Physics, Centre for the Study of Neurological Disorders, Microsurgical Research and Training Facility, RCSI, Dublin 2, Ireland.
⁴ Cellular and Molecular Imaging Core, RCSI, Dublin 2, Ireland.
⁵ Tissue Engineering Research Group, Department of Anatomy, Royal College of Surgeons in Ireland (RCSI), 123 St. Stephens Green, Dublin 2, Ireland; Trinity Centre for Biomedical Engineering, Trinity College Dublin (TCD), College Green, Dublin 2, Ireland; Advanced Materials and Bioengineering Research Centre (AMBER), RCSI and TCD, Dublin 2, Ireland; Anatomy, School of Medicine, College of Medicine Nursing and Health Sciences, University of Galway, University Road, Galway, Ireland.
⁶ Tissue Engineering Research Group, Department of Anatomy, Royal College of Surgeons in Ireland (RCSI), 123 St. Stephens Green, Dublin 2, Ireland; Trinity Centre for Biomedical Engineering, Trinity College Dublin (TCD), College Green, Dublin 2, Ireland; Advanced Materials and Bioengineering Research Centre (AMBER), RCSI and TCD, Dublin 2, Ireland. Electronic address: carolinecurtin@rcsi.ie.
⁷ Tissue Engineering Research Group, Department of Anatomy, Royal College of Surgeons in Ireland (RCSI), 123 St. Stephens Green, Dublin 2, Ireland; Trinity Centre for Biomedical Engineering, Trinity College Dublin (TCD), College Green, Dublin 2, Ireland; Advanced Materials and Bioengineering Research Centre (AMBER), RCSI and TCD, Dublin 2, Ireland. Electronic address: fjobrien@rcsi.ie.

PMID: 37797708
DOI: 10.1016/j.actbio.2023.09.049

Abstract

Angiogenesis is critical for successful bone repair, and interestingly, miR-210 and miR-16 possess counter-active targets involved in both angiogenesis and osteogenesis: miR-210 acts as an activator by silencing EFNA3 & AcvR1b, while miR-16 inhibits both pathways by silencing VEGF & Smad5. It was thus hypothesized that dual delivery of both a miR-210 mimic and a miR-16 inhibitor from a collagen-nanohydroxyapatite scaffold system may hold significant potential for bone repair. Therefore, this systems potential to rapidly accelerate bone repair by directing enhanced angiogenic-osteogenic coupling in host cells in a rat calvarial defect model at a very early 4 week timepoint was assessed. In vitro, the treatment significantly enhanced angiogenic-osteogenic coupling of human mesenchymal stem cells, with enhanced calcium deposition after just 10 days in 2D and 14 days on scaffolds. In vivo, these dual-miRNA loaded scaffolds showed more than double bone volume and vessel recruitment increased 2.3 fold over the miRNA-free scaffolds. Overall, this study demonstrates the successful development of a dual-miRNA mimic/inhibitor scaffold for enhanced in vivo bone repair for the first time, and the possibility of extending this 'off-the-shelf' platform system to applications beyond bone offers immense potential to impact a myriad of other tissue engineering areas. STATEMENT OF SIGNIFICANCE: miRNAs have potential as a new class of bone healing therapeutics as they can enhance the regenerative capacity of bone-forming cells. However, angiogenic-osteogenic coupling is critical for successful bone repair. Therefore, this study harnesses the delivery of miR-210, known to be an activator of both angiogenesis and osteogenesis, and miR-16 inhibitor, as miR-16 is known to inhibit both pathways, from a collagen-nanohydroxyapatite scaffold system to rapidly enhance osteogenesis in vitro and bone repair in vivo in a rat calvarial defect model. Overall, it describes the successful development of the first dual-miRNA mimic/inhibitor scaffold for enhanced in vivo bone repair. This 'off-the-shelf' platform system offers immense potential to extend beyond bone applications and impact a myriad of other tissue engineering areas.

Keywords: Angiogenesis; Bone repair; Dual delivery; Gene therapy; Nano-hydroxyapatite; Non-viral vector; Scaffold; miR-16; miR-210; microRNA.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Bone Regeneration
Bone and Bones / metabolism
Cell Differentiation
Collagen
Humans
MicroRNAs* / genetics
MicroRNAs* / metabolism
Osteogenesis* / genetics
Rats
Tissue Engineering
Tissue Scaffolds

Substances

MicroRNAs
Collagen
MIRN16 microRNA, human
MIRN210 microRNA, human
MIRN16 microRNA, rat
MIRN210 microRNA, rat