## Abstract A novel synthetic peptide corresponding to BMP‐2 residues 73–92 that can induce bone formation and can form a conjugate with a carrier to localize its effect has been reported previously. The synthetic peptide was bound to a BMP‐2–specific receptor, and it elevated both the alkaline pho
Reconstruction of peri-implant bone defects using impacted bone allograft and BMP-2 gene-modified bone marrow stromal cells
✍ Scribed by Meng-Ning Yan; Ke-Rong Dai; Ting-Ting Tang; Zhen-An Zhu; Jue-Ren Lou
- Publisher
- John Wiley and Sons
- Year
- 2009
- Tongue
- English
- Weight
- 435 KB
- Volume
- 9999A
- Category
- Article
- ISSN
- 1549-3296
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✦ Synopsis
Abstract
Impaction bone allografting represents an attractive procedure for bone defects reconstruction in joint replacement. And it was found that bone morphogenetic protein‐2(BMP‐2) gene therapy can enhance bone healing. The purpose of this study was to determine if combined adenovirus mediated human BMP‐2(Adv‐hBMP‐2) gene‐modified bone marrow stromal cells(BMSCs) with allograft enhanced the defects healing and improved the strength of implant fixation in 3‐mm bone defect around a titanium alloy implant. Using the impaction grafting technique, the defects were reconstructed using freeze‐dried allograft, freeze‐dried allografts loaded with autogenous BMSCs, or freeze‐dried allografts loaded with autogenous BMSCs modified with the human bone morphogenetic protein‐2 (hBMP‐2) gene. At 6 and 12 weeks, the Bone‐implant Contact rate and strength of the interface in the group with BMP‐2 gene medication were significantly higher than those of the non‐cell or cell groups. BMP‐2 gene medication also showed significant effects on allograft healing and replacement compared with those of two other groups, as evidenced by increased new bone formation and reduced graft remnants. The results suggest that BMP‐2 gene medication can enhance allograft healing and osseointegration of the bone‐implant interface. © 2009 Wiley Periodicals, Inc. J Biomed Mater Res 2010
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