Oxidized alginate hydrogels for bone morphogenetic protein-2 delivery in long bone defects

[Display omitted] Autograft treatment of large bone defects and fracture non-unions is complicated by limited tissue availability and donor site morbidity. Polymeric biomaterials such as alginate hydrogels provide an attractive tissue engineering alternative due to their biocompatibility, injectabil...

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Bibliographic Details
Published in:Acta biomaterialia 2014-10, Vol.10 (10), p.4390-4399
Main Authors: Priddy, Lauren B., Chaudhuri, Ovijit, Stevens, Hazel Y., Krishnan, Laxminarayanan, Uhrig, Brent A., Willett, Nick J., Guldberg, Robert E.
Format: Article
Language:English
Subjects:
Alginate
Alginates
Alginates - chemistry
Alginates - pharmacology
Animals
Bioactivity
Biocompatibility
BMP-2 (bone morphogenetic protein-2)
Bone Morphogenetic Protein 2 - chemistry
Bone Morphogenetic Protein 2 - pharmacology
Bone regeneration
Bone Regeneration - drug effects
Bones
Cell Line
Defects
Degradation
Disease Models, Animal
Drug Delivery Systems
Female
Femur - abnormalities
Femur - pathology
Glucuronic Acid - chemistry
Glucuronic Acid - pharmacology
Hexuronic Acids - chemistry
Hexuronic Acids - pharmacology
Humans
Hydrogels
Hydrogels - chemistry
Hydrogels - pharmacology
Irradiation
Mice
Oxidation
Oxidation-Reduction
Rats
Rats, Sprague-Dawley
Surgical implants
Time Factors
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Summary:[Display omitted] Autograft treatment of large bone defects and fracture non-unions is complicated by limited tissue availability and donor site morbidity. Polymeric biomaterials such as alginate hydrogels provide an attractive tissue engineering alternative due to their biocompatibility, injectability, and tunable degradation rates. Irradiated RGD-alginate hydrogels have been used to deliver proteins such as bone morphogenetic protein-2 (BMP-2), to promote bone regeneration and restoration of function in a critically sized rat femoral defect model. However, slow degradation of irradiated alginate hydrogels may impede integration and remodeling of the regenerated bone to its native architecture. Oxidation of alginate has been used to promote degradation of alginate matrices. The objective of this study was to evaluate the effects of alginate oxidation on BMP-2 release and bone regeneration. We hypothesized that oxidized-irradiated alginate hydrogels would elicit an accelerated release of BMP-2, but degrade faster in vivo, facilitating the formation of higher quality, more mature bone compared to irradiated alginate. Indeed, oxidation of irradiated alginate did accelerate in vitro BMP-2 release. Notably, the BMP-2 retained within both constructs was bioactive at 26days, as observed by induction of alkaline phosphatase activity and positive Alizarin Red S staining of MC3T3-E1 cells. From the in vivo study, robust bone regeneration was observed in both groups through 12weeks by radiography, micro-computed tomography analyses, and biomechanical testing. Bone mineral density was significantly greater for the oxidized-irradiated alginate group at 8weeks. Histological analyses of bone defects revealed enhanced degradation of oxidized-irradiated alginate and suggested the presence of more mature bone after 12weeks of healing.
ISSN:1742-7061
1878-7568
DOI:10.1016/j.actbio.2014.06.015