Grand Rapids Medical Education Partners, 1000 Monroe Ave NW, Grand Rapids, MI 48195, USA; Department of Surgery, BG-University Hospital Bergmannsheil, Bürkle-de-la-Camp-Platz 1, 44789 Bochum, Germany.
Spine J. 2013 Oct;13(10):1244-52. doi: 10.1016/j.spinee.2013.06.022. Epub 2013 Aug 22.
Recombinant human bone morphogenetic protein-2 (rhBMP-2) (INFUSE, Medtronic, Memphis, TN, USA) has been used off-label for posterolateral lumbar fusions for many years.
The goal of this study was to evaluate the complications requiring reoperation associated with rhBMP-2 application for posterolateral lumbar fusions.
STUDY DESIGN/SETTING: During a 7-year period of time (2002-2009), all patients undergoing lumbar posterolateral fusion using rhBMP-2 (INFUSE) were retrospectively evaluated within a large orthopedic surgery private practice.
A total of 1,158 consecutive patients were evaluated with 468 (40.4%) males and 690 (59.6%) females.
Complications related to rhBMP were defined as reoperation secondary to symptomatic failed fusion (nonunion), symptomatic seroma formation, symptomatic reformation of foraminal bone, and infection.
Inclusion criteria were posterolateral fusion with rhBMP-2 implant and age equal to or older than 18 years. Surgical indications and treatment were performed in accordance with the surgeon's best knowledge, discretion, and experience. Patients consented to lumbar decompression and arthrodesis using rhBMP-2. All patients were educated and informed of the off-label utilization of rhBMP-2. Patient follow-up was performed at regular intervals of 2 weeks, 6 weeks, 12 weeks, 6 months, 1 year, and later if required or indicated.
Average age was 59.2 years, and body mass index was 30.7 kg/m². Numbers of levels fused were 1 (414, 35.8%), 2 (469, 40.5%), 3 (162, 14.0%), 4 (70, 6.0%), 5 (19, 1.6%), 6 (11, 0.9%), 7 (7, 0.6%), 8 (4, 0.3%), and 9 (2, 0.2%). Patients having complications requiring reoperation were 117 of 1,158 (10.1%): symptomatic nonunion requiring redo fusion and instrumentation 41 (3.5%), seroma with acute neural compression 32 (2.8%), excess bone formation with delayed neural compression 4 (0.3%), and infection requiring debridement 26 (2.2%). Nonunion was related to male sex and previous BMP exposure. Seroma formation was significantly higher in patients with higher doses of rhBMP-2 (p=.050) and with more than 12 mg of rhBMP-2 (χ(2)=0.025). Bone reformation and neural compression at the laminectomy and foraminotomy sites occurred in a delayed fashion. Infection was associated with obesity and respiratory disease. Infections were noted with a greater BMP dose (p<.001), more than 12 mg (χ(2)<0.001), fusion more than three levels (χ(2)<0.001), and reexposed to BMP (χ(2)=0.023).
rhBMP-2 utilization for posterolateral lumbar fusions has a low symptomatic nonunion rate. Prior rhBMP-2 exposure and male sex were related to symptomatic nonunion formation. rhBMP-2-associated neural compression acutely with seroma formation and delayed with foraminal bone formation is concerning and associated with higher rhBMP-2 concentrations.
重组人骨形态发生蛋白-2(rhBMP-2)(INFUSE,美敦力,田纳西州孟菲斯)多年来一直被非适应证用于后路腰椎融合术。
本研究旨在评估与 rhBMP-2 用于后路腰椎融合术相关的需要再次手术的并发症。
研究设计/设置:在 7 年期间(2002-2009 年),在一家大型骨科私人诊所对使用 rhBMP-2(INFUSE)进行后路腰椎融合术的所有患者进行了回顾性评估。
共评估了 1158 例连续患者,其中 468 例(40.4%)为男性,690 例(59.6%)为女性。
与 rhBMP 相关的并发症定义为因症状性融合失败(非融合)、症状性血清肿形成、症状性再形成椎间孔骨和感染而需要再次手术。
纳入标准为后路融合术使用 rhBMP-2 植入物,年龄等于或大于 18 岁。手术指征和治疗均根据外科医生的最佳知识、判断力和经验进行。患者同意使用 rhBMP-2 进行腰椎减压和融合术。所有患者均接受了 rhBMP-2 非适应证使用的教育和告知。患者随访在定期的 2 周、6 周、12 周、6 个月、1 年及以后进行,如果需要或需要。
平均年龄为 59.2 岁,体重指数为 30.7kg/m²。融合的节段数为 1 个(414 例,35.8%)、2 个(469 例,40.5%)、3 个(162 例,14.0%)、4 个(70 例,6.0%)、5 个(19 例,1.6%)、6 个(11 例,0.9%)、7 个(7 例,0.6%)、8 个(4 例,0.3%)和 9 个(2 例,0.2%)。需要再次手术的并发症患者为 117 例(10.1%):需要再次融合和器械固定的症状性非融合 41 例(3.5%)、急性神经压迫的血清肿 32 例(2.8%)、延迟性神经压迫的过度骨形成 4 例(0.3%)和需要清创的感染 26 例(2.2%)。非融合与男性性别和先前的 BMP 暴露有关。血清肿形成与 rhBMP-2 剂量较高(p=.050)和 rhBMP-2 超过 12mg(χ(2)=0.025)显著相关。骨形成和在椎板切除术和椎间孔切开术部位的神经压迫发生延迟。感染与肥胖和呼吸道疾病有关。感染与较大的 BMP 剂量(p<.001)、超过 12mg(χ(2)<0.001)、超过三个节段的融合(χ(2)<0.001)和再次暴露于 BMP(χ(2)=0.023)有关。
后路腰椎融合术使用 rhBMP-2 的症状性非融合率较低。先前的 rhBMP-2 暴露和男性性别与症状性非融合形成有关。与 rhBMP-2 相关的急性血清肿形成和延迟性椎间孔骨形成的神经压迫令人关注,并与较高的 rhBMP-2 浓度有关。
