Gene activated scaffolds incorporating star-shaped polypeptide-pDNA nanomedicines accelerate bone tissue regeneration in vivo

David P. Walsh; Rosanne M. Raftery; Robert Murphy; Gang Chen; Andreas Heise; Fergal J. O'Brien; Sally-Ann Cryan

doi:10.1039/D1BM00094B

Gene activated scaffolds incorporating star-shaped polypeptide-pDNA nanomedicines accelerate bone tissue regeneration in vivo†

David P. Walsh,

^abcd Rosanne M. Raftery,

^bcd Robert Murphy,^e Gang Chen,^f Andreas Heise,

^deg Fergal J. O'Brien^abcdg and Sally-Ann Cryan

*^abcg

Author affiliations

* Corresponding authors

^a Drug Delivery & Advanced Materials Team, School of Pharmacy & Biomolecular Sciences, RCSI, Dublin, Ireland

^b Tissue Engineering Research Group, Department of Anatomy & Regenerative Medicine, RCSI, Dublin, Ireland

^c Trinity Centre for Biomedical Engineering, Trinity College Dublin (TCD), Dublin, Ireland

^d SFI Advanced Materials and Bioengineering Research (AMBER) Centre, RCSI & TCD, Ireland

^e Department of Chemistry, RCSI, Dublin, Ireland

^f Centre for the Study of Neurological Disorders, Microsurgical Research and Training Facility (MRTF), RCSI, Dublin, Ireland

^g SFI Centre for Research in Medical Devices (CURAM), RCSI, Dublin and National University of Ireland, Galway, Ireland

Abstract

Increasingly, tissue engineering strategies such as the use of biomaterial scaffolds augmented with specific biological cues are being investigated to accelerate the regenerative process. For example, significant clinical challenges still exist in efficiently healing large bone defects which are above a critical size. Herein, we describe a cell-free, biocompatible and bioresorbable scaffold incorporating a novel star-polypeptide biomaterial as a gene vector. This gene-loaded scaffold can accelerate bone tissue repair in vivo in comparison to a scaffold alone at just four weeks post implantation in a critical sized bone defect. This is achieved via the in situ transfection of autologous host cells which migrate into the implanted collagen-based scaffold via gene-loaded, star-shaped poly(L-lysine) polypeptides (star-PLLs). In vitro, we demonstrate that star-PLL nanomaterials designed with 64 short poly(L-lysine) arms can be used to functionalise a range of collagen based scaffolds with a dual therapeutic cargo (pDual) of the bone-morphogenetic protein-2 plasmid (pBMP-2) and vascular endothelial growth factor plasmid (pVEGF). The versatility of this polymeric vector is highlighted in its ability to transfect Mesenchymal Stem Cells (MSCs) with both osteogenic and angiogenic transgenes in a 3D environment from a range of scaffolds with various macromolecular compositions. In vivo, we demonstrate that a bone-mimetic, collagen-hydroxyapatite scaffold functionalized with star-PLLs containing either 32- or 64- poly(L-lysine) arms can be used to successfully deliver this pDual cargo to autologous host cells. At the very early timepoint of just 4 weeks, we demonstrate the 64-star-PLL-pDual functionalised scaffold as a particularly efficient platform to accelerate bone tissue regeneration, with a 6-fold increase in new bone formation compared to a scaffold alone. Overall, this article describes for the first time the incorporation of novel star-polypeptide biomaterials carrying two therapeutic genes into a cell free scaffold which supports accelerated bone tissue formation in vivo.

This article is part of the themed collection: Biomaterials Science Most Popular 2021

Biomaterials Science

Gene activated scaffolds incorporating star-shaped polypeptide-pDNA nanomedicines accelerate bone tissue regeneration in vivo†

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Gene activated scaffolds incorporating star-shaped polypeptide-pDNA nanomedicines accelerate bone tissue regeneration in vivo

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