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Heparin-mediated delivery of bone morphogenetic protein-2 improves spatial localization of bone regeneration.


ABSTRACT: Supraphysiologic doses of bone morphogenetic protein-2 (BMP-2) are used clinically to promote bone formation in fracture nonunions, large bone defects, and spinal fusion. However, abnormal bone formation (i.e., heterotopic ossification) caused by rapid BMP-2 release from conventional collagen sponge scaffolds is a serious complication. We leveraged the strong affinity interactions between heparin microparticles (HMPs) and BMP-2 to improve protein delivery to bone defects. We first developed a computational model to investigate BMP-2-HMP interactions and demonstrated improved in vivo BMP-2 retention using HMPs. We then evaluated BMP-2-loaded HMPs as a treatment strategy for healing critically sized femoral defects in a rat model that displays heterotopic ossification with clinical BMP-2 doses (0.12 mg/kg body weight). HMPs increased BMP-2 retention in vivo, improving spatial localization of bone formation in large bone defects and reducing heterotopic ossification. Thus, HMPs provide a promising opportunity to improve the safety profile of scaffold-based BMP-2 delivery.

SUBMITTER: Hettiaratchi MH 

PROVIDER: S-EPMC6941907 | biostudies-literature | 2020 Jan

REPOSITORIES: biostudies-literature

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Heparin-mediated delivery of bone morphogenetic protein-2 improves spatial localization of bone regeneration.

Hettiaratchi Marian H MH   Krishnan Laxminarayanan L   Rouse Tel T   Chou Catherine C   McDevitt Todd C TC   Guldberg Robert E RE  

Science advances 20200103 1


Supraphysiologic doses of bone morphogenetic protein-2 (BMP-2) are used clinically to promote bone formation in fracture nonunions, large bone defects, and spinal fusion. However, abnormal bone formation (i.e., heterotopic ossification) caused by rapid BMP-2 release from conventional collagen sponge scaffolds is a serious complication. We leveraged the strong affinity interactions between heparin microparticles (HMPs) and BMP-2 to improve protein delivery to bone defects. We first developed a co  ...[more]

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