* Central Growth Factor Loaded Depots in Bone Tissue Engineering Scaffolds for Enhanced Cell Attraction

Mandy Quade; Sven Knaack; Ashwini Rahul Akkineni; Anastasia Gabrielyan; Anja Lode; Angela Rösen-Wolff; Michael Gelinsky

doi:10.1089/ten.TEA.2016.0483

^* Central Growth Factor Loaded Depots in Bone Tissue Engineering Scaffolds for Enhanced Cell Attraction

Tissue Eng Part A. 2017 Aug;23(15-16):762-772. doi: 10.1089/ten.TEA.2016.0483. Epub 2017 Apr 20.

Authors

Mandy Quade¹, Sven Knaack¹, Ashwini Rahul Akkineni¹, Anastasia Gabrielyan², Anja Lode¹, Angela Rösen-Wolff², Michael Gelinsky¹

Affiliations

¹ 1 Centre for Translational Bone, Joint and Soft Tissue Research, University Hospital Carl Gustav Carus and Faculty of Medicine of Technische Universität Dresden , Dresden, Germany .
² 2 Department of Pediatrics, University Hospital Carl Gustav Carus Dresden , Dresden, Germany .

PMID: 28316275
DOI: 10.1089/ten.TEA.2016.0483

Abstract

Tissue engineering, the application of stem and progenitor cells in combination with an engineered extracellular matrix, is a promising strategy for bone regeneration. However, its success is limited by the lack of vascularization after implantation. The concept of in situ tissue engineering envisages the recruitment of cells necessary for tissue regeneration from the host environment foregoing ex vivo cell seeding of the scaffold. In this study, we developed a novel scaffold system for enhanced cell attraction, which is based on biomimetic mineralized collagen scaffolds equipped with a central biopolymer depot loaded with chemotactic agents. In humid milieu, as after implantation, the signaling factors are expected to slowly diffuse out of the central depot forming a gradient that stimulates directed cell migration toward the scaffold center. Heparin, hyaluronic acid, and alginate have been shown to be capable of depot formation. By using vascular endothelial growth factor (VEGF) as model factor, it was demonstrated that the release kinetics can be adjusted by varying the depot composition. While alginate and hyaluronic acid are able to reduce the initial burst and prolong the release of VEGF, the addition of heparin led to a much stronger retention that resulted in an almost linear release over 28 days. The biological activity of released VEGF was proven for all variants using an endothelial cell proliferation assay. Furthermore, migration experiments with endothelial cells revealed a relationship between the degree of VEGF retention and migration distance: cells invaded deepest in scaffolds containing a heparin-based depot indicating that the formation of a steep gradient is crucial for cell attraction. In conclusion, this novel in situ tissue engineering approach, specifically designed to recruit and accommodate endogenous cells upon implantation, appeared highly promising to stimulate cell invasion, which in turn would promote vascularization and finally new bone formation.

Keywords: VEGF; alginate; collagen; endothelial cells; heparin; hyaluronic acid.

Publication types

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

MeSH terms

Animals
Biomimetic Materials / pharmacology
Biopolymers / pharmacology
Bone and Bones / drug effects
Bone and Bones / physiology*
Calcification, Physiologic / drug effects
Cattle
Cell Movement / drug effects
Endothelial Cells / drug effects
Endothelial Cells / metabolism
Humans
Tissue Engineering / methods*
Tissue Scaffolds / chemistry*
Vascular Endothelial Growth Factor A / pharmacology*

Substances

Biopolymers
Vascular Endothelial Growth Factor A