首页> 美国卫生研究院文献>Materials >Reduction of Adipose Tissue Formation by the Controlled Release of BMP-2 Using a Hydroxyapatite-Coated Collagen Carrier System for Sinus-Augmentation/Extraction-Socket Grafting
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Reduction of Adipose Tissue Formation by the Controlled Release of BMP-2 Using a Hydroxyapatite-Coated Collagen Carrier System for Sinus-Augmentation/Extraction-Socket Grafting

机译:使用羟基磷灰石涂层胶原蛋白载体系统通过窦性增强/拔牙窝接枝术控制释放BMP-2来减少脂肪组织的形成

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摘要

The effects of hydroxyapatite (HA)-coating onto collagen carriers for application of recombinant human bone morphogenetic protein 2 (rhBMP-2) on cell differentiation in vitro, and on in vivo healing patterns after sinus-augmentation and alveolar socket-grafting were evaluated. In vitro induction of osteogenic/adipogenic differentiation was compared between the culture media with rhBMP-2 solution and with the released rhBMP-2 from the control collagen and from the HA-coated collagen. Demineralized bovine bone and collagen/HA-coated collagen were grafted with/without rhBMP-2 in sinus-augmentation and tooth-extraction-socket models. Adipogenic induction by rhBMP-2 released from HA-coated collagen was significantly reduced compared to collagen. In the sinus-augmentation model, sites that received rhBMP-2 exhibited large amounts of vascular tissue formation at two weeks and increased adipose tissue formation at eight weeks; this could be significantly reduced by using HA-coated collagen as a carrier for rhBMP-2. In extraction-socket grafting, dimensional reduction of alveolar ridge was significantly decreased at sites received rhBMP-2 compared to control sites, but adipose tissue was increased within the regenerated socket area. In conclusion, HA-coated collagen carrier for Escherichia coli-derived rhBMP-2 (ErhBMP-2) may reduce in vitro induction of adipogenic differentiation and in vivo adipose bone marrow tissue formation in bone tissue engineering by ErhBMP-2.
机译:评估了羟基磷灰石(HA)涂层在胶原蛋白载体上的应用,该重组胶原蛋白用于重组人骨形态发生蛋白2(rhBMP-2)在体外对细胞分化的影响以及对鼻窦增强和牙槽窝移植后体内愈合模式的影响。在具有rhBMP-2溶液的培养基与从对照胶原和从HA包被的胶原中释放的rhBMP-2之间,比较了体外诱导成骨/成脂分化的方法。在窦扩张和拔牙窝模型中,将脱矿质的牛骨和胶原蛋白/ HA包被的胶原蛋白移植有/没有rhBMP-2。与胶原蛋白相比,由HA包被的胶原蛋白释放的rhBMP-2引起的成脂诱导明显减少。在窦扩张模型中,接受rhBMP-2的位点在两周时显示出大量的血管组织形成,而在八周时则显示出增加的脂肪组织形成。通过使用HA包被的胶原蛋白作为rhBMP-2的载体,可以显着降低这种情况。在拔牙窝移植中,与对照位点相比,在接受rhBMP-2的位点,牙槽的尺寸减小明显减少,但是在再生的窝区内,脂肪组织增加。总之,用于大肠杆菌的rhBMP-2(ErhBMP-2)的HA包被的胶原蛋白载体可减少ErhBMP-2在骨组织工程中体外诱导的成脂分化和体内脂肪骨髓组织形成。

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