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Evaluation of insoluble bone gelatin as a carrier for enhancement of osteogenic protein-1-induced intertransverse process lumbar fusion in a rabbit model.

机译:评估不溶性骨明胶作为载体增强兔模型中成骨蛋白-1诱导的横突间腰椎融合的方法。

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STUDY DESIGN: Postero-lateral lumbar fusion in a rabbit model was performed to compare the bone induction potential of autograft, insoluble bone gelatin (ISBG), osteogenic protein-1 (OP-1), and the combination of ISBG and OP-1. OBJECTIVE: To evaluate the efficiency of ISBG as a carrier/enhancer for OP-1 in a rabbit spinal fusion model. SUMMARY OF BACKGROUND DATA: OP-1 or recombinant human BMP-7 has been shown to be effective in inducing new bone formation in surgical applications such as spinal arthrodesis. However, the lack of an ideal carrier contributes to its associated comorbidities (e.g., uncontrolled bone growth, local inflammatory over-response, nonfusion) and limits its use clinically. METHODS: Adult New Zealand white rabbits (n = 32) underwent bilateral lumbar intertransverse process fusion procedures at L5 to L6 and were randomized to receive: (1) autograft; (2) ISBG; (3) OP-1; or (4) ISBG in combination with OP-1 (ISBG + OP-1). Spinal fusion masses were evaluated by manual palpation, biomechanical testing, radiographic assessment, microcomputer tomography scanning and histologic examination at 6 weeks after surgery. RESULTS: Treatment of ISBG + OP-1 resulted in higher spinal fusion rates (7 of 7, 100%) than that of autograft (3 of 7, 43%), ISBG (2 of 8, 25%), and OP-1 (2 of 7, 29%) based on manual palpation (P < 0.01). Greater fusion rates in the ISBG + OP-1 group were also evidenced by radiographic examination (P < 0.01), microcomputer tomography bone volume analysis (P < 0.01), and biomechanical testing (P < 0.05). Histologic assessment demonstrated that treatment of ISBG + OP-1 induces new contiguous bone formation in the interval between the transverse processes which was absent in the other groups. CONCLUSION: In this study, ISBG + OP-1 resulted in more effective lumbar intertransverse process fusion than autograft, OP-1 putty or ISBG alone. ISBG is capable of enhancing OP-1-induced bone formation.
机译:研究设计:在兔模型中进行后外侧腰椎融合术,比较自体移植物,不溶性骨明胶(ISBG),成骨蛋白1(OP-1)以及ISBG和OP-1组合的骨诱导潜力。目的:评估ISBG作为兔脊柱融合模型中OP-1的载体/增强剂的效率。背景数据概述:OP-1或重组人BMP-7已被证明在诸如脊椎关节固定术等外科手术应用中有效诱导新的骨形成。然而,缺乏理想的载体会导致其相关的合并症(例如,骨生长不受控制,局部炎症过度反应,不融合),并限制了其临床应用。方法:成年新西兰白兔(n = 32)在L5至L6接受双侧腰间横突融合术,并随机接受:(1)自体移植; (2)ISBG; (3)OP-1;或(4)ISBG与OP-1(ISBG + OP-1)组合。术后6周通过手触诊,生物力学测试,影像学评估,微型计算机断层扫描和组织学检查对脊柱融合肿块进行评估。结果:ISBG + OP-1的治疗导致的脊柱融合率(7/7,100%)高于自体移植(3/7,43%),ISBG(2/8,25%)和OP-1 (7之2,占29%)基于手动触诊(P <0.01)。 ISBG + OP-1组的融合率更高,还通过放射线照相检查(P <0.01),微型计算机断层扫描骨体积分析(P <0.01)和生物力学测试(P <0.05)证明。组织学评估表明,对ISBG + OP-1的治疗在横突之间的间隔中诱导了新的连续骨形成,而其他组则没有。结论:在这项研究中,ISBG + OP-1比单独使用自体移植物,OP-1油灰或ISBG产生更有效的腰间横突融合术。 ISBG能够增强OP-1诱导的骨形成。

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