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首页> 外文期刊>Journal of Periodontology >Recombinant human bone morphogenetic protein-2 stimulation of bone formation around endosseous dental implants.
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Recombinant human bone morphogenetic protein-2 stimulation of bone formation around endosseous dental implants.

机译:重组人骨形态发生蛋白2刺激骨内牙种植体周围骨形成。

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摘要

BACKGROUND: Successful endosseous implant placement requires that the implant be stable in alveolar bone. In certain cases, the implant can be stabilized in native bone but some part of the implant is not covered by bone tissue. This often occurs during placement of implants into extraction sites or in areas where bone resorption has occurred and the ridge width is not sufficient to completely surround the implant. In those cases, the clinician usually employs a procedure to encourage bone formation. These procedures typically include a bone graft and/or membrane therapy. Recent advances have led to the isolation, cloning, and production of recombinant human proteins that stimulate bone formation. One of these bone morphogenetic proteins (rhBMP-2) has been extensively studied in animal models and is currently being tested in human clinical trials. METHODS: In this study, rhBMP-2 was tested using a collagen sponge carrier to stimulate bone formation in defects in the canine mandible around endosseous dental implants. Six animals had a total of 48 implants placed. rhBMP-2 with the collagen carrier was implanted around 24 of these, the remainder having only the collagen carrier placed. Half the sites were covered with a nonresorbable expanded polytetrafluoroethylene membrane. Histologic analysis was performed after 4 and 12 weeks. The area of new bone formed, percentage of bone-to-implant contact in the defect area, and percentage fill of the defect was calculated. RESULTS: The addition of rhBMP-2 resulted in significantly greater amounts of new bone area and percentage of bone-to-implant contact and with more percentage fill after 4 and 12 weeks of healing. The area of new bone formed was reduced after 4 weeks when a membrane was present but after 12 weeks, there was no significant difference between membrane and non-membrane treated sites. In some specimens, new bone was found coronal to the membranes, with rhBMP-2-treated sites having greater amounts than non-rhBMP-2-treated sites. CONCLUSIONS: These data demonstrate that a bone differentiation factor significantly stimulates bone formation in peri-implant bone defects in the canine mandible. In addition, bone-to-implant contact was significantly enhanced along the rough implant surface. Membrane-treated sites had less new bone formation after 4 weeks of healing but were similar to non-membrane sites after 12 weeks. These results demonstrate that rhBMP-2 can be used to stimulate bone growth both around and onto the surface of endosseous dental implants placed in sites with extended peri-implant osseous defects.
机译:背景:成功植入骨内植入物要求植入物在牙槽骨中稳定。在某些情况下,植入物可以稳定在天然骨中,但是植入物的某些部分没有被骨组织覆盖。这通常发生在将植入物放置到拔除部位或发生骨吸收并且脊宽度不足以完全包围植入物的区域中。在这些情况下,临床医生通常采用一种程序来鼓励骨形成。这些程序通常包括骨移植和/或膜疗法。最近的进展已导致刺激骨形成的重组人蛋白质的分离,克隆和生产。这些骨形态发生蛋白(rhBMP-2)之一已在动物模型中进行了广泛研究,目前正在人类临床试验中进行测试。方法:在这项研究中,使用胶原蛋白海绵载体对rhBMP-2进行了测试,以刺激骨内牙植入物周围犬下颌骨缺损的骨形成。六只动物总共放置了48个植入物。将其中带有胶原蛋白载体的rhBMP-2植入其中的24个,其余仅放置胶原蛋白载体。一半的部位被不可吸收的膨胀聚四氟乙烯膜覆盖。在4和12周后进行组织学分析。计算出新骨形成的面积,缺损区域中骨与植入物的接触百分比以及缺损的填充百分比。结果:rhBMP-2的添加导致愈合后4周和12周的新骨面积和骨与植入物接触的百分比显着增加,并且填充的百分比更高。存在膜后4周后,新骨形成的面积减少,但在12周后,膜和非膜处理部位之间没有显着差异。在一些标本中,发现新的骨头位于膜冠状,rhBMP-2处理的部位比未rhBMP-2处理的部位多。结论:这些数据表明骨分化因子显着刺激犬下颌骨种植体周围骨缺损中的骨形成。此外,沿着粗糙的种植体表面,骨骼与种植体的接触得到了显着增强。膜处理的部位在愈合4周后具有较少的新骨形成,但与12周后的非膜部位相似。这些结果表明,rhBMP-2可用于刺激骨内种植体周围和表面的骨生长,这些种植体位于种植体周围骨缺损扩展的部位。

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