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Simple carrier matrix modifications can enhance delivery of recombinant human bone morphogenetic protein-2 for posterolateral spine fusion.

机译:简单的载体基质修饰可以增强重组人骨形态发生蛋白2用于后外侧脊柱融合的递送。

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STUDY DESIGN: A nonhuman primate lumbar intertransverse process arthrodesis model was used to evaluate modifications to a plain collagen sponge to deliver recombinant human bone morphogenetic protein-2 (rhBMP-2). OBJECTIVES: To evaluate the feasibility of enhancing the delivery of rhBMP-2 with the established collagen sponge carrier by adding biphasic ceramic phosphate (BCP) granules (15% hydroxyapatite, 85% tricalcium phosphate) or allograft chips to provide compression resistance for posterolateral spine arthrodesis. SUMMARY OF BACKGROUND DATA: Recombinant human bone morphogenetic protein-2 was successfully delivered with a resorbable collagen sponge in a rabbit intertransverse process fusion model. Success in nonhuman primates required a higher dose (6-9 mg) of rhBMP-2 and a more compression-resistant matrix (ceramic) than plain collagen. The limitation of the ceramic carrier was its radiopacity, which made radiographic detection of new bone formation difficult. METHODS: Nine adult rhesus monkeys underwent bilateral posterolateral intertransverse process arthrodesis at L4-L5. The animals were divided into three groups (n = 3 each) based on the graft material implanted: 1) autogenous iliac crest bone (5 cm3/side); 2) collagen sponge and 15:85 BCP granules loaded with rhBMP-2 (3 mg/side); and, 3) collagen sponge and allograft chips loaded with rhBMP-2 (3 mg/side). The monkeys were killed 24 weeks after surgery. Inspection, manual palpation, radiography, computed tomographic scans, and histology were used to assess fusion. RESULTS: All six monkeys with rhBMP-2 delivered in the collagen/15:85 BCP carrier and the collagen/allograft chips carrier achieved solid spine fusions, whereas only one of three animals fused with autogenous bone graft. Histologic analysis of the bone induced by rhBMP-2 showed normal trabecular bone and bone marrow elements. CONCLUSIONS: The addition of either 15:85 BCP granules or allograft bone chips to the existing resorbable collagen sponge matrix enhanced delivery of rhBMP-2 in the posterolateral spine. The combination matrices were more compression resistant and had improved radiographic resorption properties that permitted easy radiographic visualization of new bone. In addition, a lower dose of rhBMP-2 (3 mg/side) was successful compared with the dose previously used with the plain collagen sponge (6 mg/side).
机译:研究设计:非人灵长类动物腰间横突关节固定术模型用于评估对普通胶原蛋白海绵的修饰,以提供重组人骨形态发生蛋白2(rhBMP-2)。目的:通过添加双相陶瓷磷酸盐(BCP)颗粒(15%羟基磷灰石,85%磷酸三钙)或同种异体移植片为后外侧脊柱关节置换术提供抗压性,评估用已建立的胶原蛋白海绵载体增强rhBMP-2递送的可行性。背景数据摘要:重组人骨形态发生蛋白2与可吸收的胶原海绵在兔子的横向过程融合模型中成功传递。非人类灵长类动物的成功需要比普通胶原蛋白更高的剂量(6-9 mg)的rhBMP-2和更耐压的基质(陶瓷)。陶瓷载体的局限性在于其射线不透性,这使得射线照相难以检测出新骨的形成。方法:9只成年恒河猴在L4-L5接受双侧后外侧横突关节固定术。根据植入的移植材料将动物分为三组(每组n = 3):1)自体骨骨(5 cm3 /侧); 2)胶原蛋白海绵和15:85 BCP颗粒,其中装有rhBMP-2(3 mg /侧); 3)装有rhBMP-2(3 mg /侧)的胶原蛋白海绵和同种异体移植芯片。手术后24周将猴子杀死。检查,人工触诊,放射线照相,计算机断层扫描和组织学用于评估融合。结果:所有六只在胶原蛋白/ 15:85 BCP载体和胶原蛋白/同种异体移植芯片载体中均带有rhBMP-2的猴子实现了牢固的脊柱融合,而三只动物中只有一只融合了自体骨移植物。 rhBMP-2诱导的骨组织学分析显示正常的小梁骨和骨髓成分。结论:向现有的可吸收胶原海绵基质中添加15:85 BCP颗粒或同种异体骨碎片可增强rhBMP-2在后外侧脊柱中的递送。组合基质具有更高的抗压性,并具有改进的射线照相吸收特性,从而可以轻松地对新骨进行射线照相可视化。此外,与以前使用普通胶原蛋白海绵的剂量(6 mg /侧)相比,成功降低了rhBMP-2剂量(3 mg /侧)。

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