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Modulating hydrogel crosslink density and degradation to control bone morphogenetic protein delivery and in vivo bone formation.

J Control Release.. 2014-06; 
JL Holloway, H Ma, R Rai, JA Burdick. 210 S 33rd St, Skirkanich Hall Rm. 240, University of Pennsylvania, Philadelphia 19104, USA.
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摘要

Bone morphogenetic proteins (BMPs) show promise in therapies for improving bone formation after injury; however, the high supraphysiological concentrations required for desired osteoinductive effects, off-target concerns, costs, and patient variability have limited the use of BMP-based therapeutics. To better understand the role of biomaterial design in BMP delivery, a matrix metalloprotease (MMP)-sensitive hyaluronic acid (HA)-based hydrogel was used for BMP-2 delivery to evaluate the influence of hydrogel degradation rate on bone repair in vivo. Specifically, maleimide-modified HA (MaHA) macromers were crosslinked with difunctional MMP-sensitive peptides to permit protease-mediated hydrogel degradation and gr... More

关键词

Bone morphogenetic protein; Bone repair; Calvarial defect; Hyaluronic acid; Hydrogel