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Homogeneous osteogenesis and bone regeneration by demineralized bone matrix loading with collagen-targeting bone morphogenetic protein-2.

机译:均质的成骨作用和骨骼再生,方法是将脱矿骨基质负载胶原蛋白靶向性骨形态发生蛋白2。

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摘要

Considerable research has been focused on the development of bone morphogenetic protein-2 (BMP-2) delivery system for homologous and efficient bone regeneration. The aim of the present study was to develop a collagen-based targeting bone repair system. A collagen-binding domain (CBD) was added to the N-terminal of native BMP-2 to allow it bind to collagen specifically. We showed that the collagen-binding bone morphogenetic protein-2 (named bone morphogenetic protein2-h, BMP2-h) had maintained the full biological activity as compared to rhBMP2 lacking the CBD. In vitro functional study also demonstrated that collagen matrix could maintain higher bioactivity of BMP2-h than native BMP-2. When demineralized bone matrix (DBM) impregnated with BMP2-h was implanted subcutaneously in rats, homogeneous bone formation was observed. Moreover, in a rabbit mandible defect model, surgical implantation of collagen matrix loaded with BMP2-h exhibited remarkable osteoinductive properties and excellent homogeneous bone formation. Our studies suggested that this novel collagen-based BMP-2 targeting bone repair system induced better bone formation not only in quantity but also in quality. Similar approaches may also be used for the repair of other tissue injuries.
机译:大量的研究集中在骨形态发生蛋白2(BMP-2)递送系统的开发上,以实现同源和有效的骨再生。本研究的目的是开发基于胶原的靶向骨修复系统。将胶原蛋白结合结构域(CBD)添加到天然BMP-2的N端,使其与胶原蛋白特异性结合。我们表明,与缺乏CBD的rhBMP2相比,胶原结合骨形态发生蛋白2(称为骨形态发生蛋白2-h,BMP2-h)具有完整的生物学活性。体外功能研究还表明,胶原蛋白基质比天然BMP-2可以维持更高的BMP2-h生物活性。当将浸渍有BMP2-h的脱矿质骨基质(DBM)皮下植入大鼠体内时,观察到均匀的骨形成。此外,在兔下颌骨缺损模型中,负载BMP2-h的胶原蛋白基质的手术植入表现出显着的骨诱导特性和出色的均匀骨形成。我们的研究表明,这种新型的基于胶原蛋白的BMP-2靶向骨修复系统不仅在数量上而且在质量上都能引起更好的骨形成。类似的方法也可以用于其他组织损伤的修复。

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