Immobilized RGD concentration and proteolytic degradation synergistically enhance vascular sprouting within hydrogel scaffolds of varying modulus

Authors

Yusheng J. He, Armour College of Engineering
Martin F. Santana, Armour College of Engineering
Madison Moucka, Department of Biological and Agricultural Engineering
Jack Quirk, Armour College of Engineering
Asma Shuaibi, Armour College of Engineering
Marja B. Pimentel, Armour College of Engineering
Sophie Grossman, Armour College of Engineering
Mudassir M. Rashid, Armour College of Engineering
Ali Cinar, Armour College of Engineering
John G. Georgiadis, Armour College of Engineering
Marcella K. Vaicik, Armour College of Engineering
Keigo Kawaji, Armour College of Engineering
David C. Venerus, Newark College of Engineering
Georgia Papavasiliou, Armour College of Engineering

Document Type

Article

Publication Date

2-11-2020

Abstract

Insufficient vascularization limits the volume and complexity of engineered tissue. The formation of new blood vessels (neovascularization) is regulated by a complex interplay of cellular interactions with biochemical and biophysical signals provided by the extracellular matrix (ECM) necessitating the development of biomaterial approaches that enable systematic modulation in matrix properties. To address this need poly(ethylene) glycol-based hydrogel scaffolds were engineered with a range of decoupled and combined variations in integrin-binding peptide (RGD) ligand concentration, elastic modulus and proteolytic degradation rate using free-radical polymerization chemistry. The modularity of this system enabled a full factorial experimental design to simultaneously investigate the individual and interaction effects of these matrix cues on vascular sprout formation in 3 D culture. Enhancements in scaffold proteolytic degradation rate promoted significant increases in vascular sprout length and junction number while increases in modulus significantly and negatively impacted vascular sprouting. We also observed that individual variations in immobilized RGD concentration did not significantly impact 3 D vascular sprouting. Our findings revealed a previously unidentified and optimized combination whereby increases in both immobilized RGD concentration and proteolytic degradation rate resulted in significant and synergistic enhancements in 3 D vascular spouting. The above-mentioned findings would have been challenging to uncover using one-factor-at-time experimental analyses.

Identifier

85076361472 (Scopus)

Publication Title

Journal of Biomaterials Science Polymer Edition

External Full Text Location

https://doi.org/10.1080/09205063.2019.1692640

e-ISSN

15685624

ISSN

09205063

PubMed ID

31774730

First Page

324

Last Page

349

Issue

3

Volume

31

Grant

EEC 1461215

Fund Ref

National Science Foundation

Recommended Citation

He, Yusheng J.; Santana, Martin F.; Moucka, Madison; Quirk, Jack; Shuaibi, Asma; Pimentel, Marja B.; Grossman, Sophie; Rashid, Mudassir M.; Cinar, Ali; Georgiadis, John G.; Vaicik, Marcella K.; Kawaji, Keigo; Venerus, David C.; and Papavasiliou, Georgia, "Immobilized RGD concentration and proteolytic degradation synergistically enhance vascular sprouting within hydrogel scaffolds of varying modulus" (2020). Faculty Publications. 5478.
https://digitalcommons.njit.edu/fac_pubs/5478