Division of Neurosurgery, Ascension Providence Hospital, Michigan State University, College of Human Medicine, Southfield, MI, USA.
Division of Neurosurgery, Ascension Providence Hospital, Michigan State University, College of Human Medicine, Southfield, MI, USA.
Spine J. 2022 Jan;22(1):8-18. doi: 10.1016/j.spinee.2021.08.011. Epub 2021 Sep 8.
Postoperative pain control following posterior lumbar fusion continues to be challenging and often requires high doses of opioids for pain relief. The use of ketorolac in spinal fusion is limited due to the risk of pseudarthrosis. However, recent literature suggests it may not affect fusion rates with short-term use and low doses.
We sought to demonstrate noninferiority regarding fusion rates in patients who received ketorolac after undergoing minimally invasive (MIS) posterior lumbar interbody fusion. Additionally, we sought to demonstrate ketorolac's opioid-sparing effect on analgesia in the immediate postoperative period.
STUDY DESIGN/SETTING: This is a prospective, randomized, double-blinded, placebo-controlled trial. We are reporting our interim analysis.
Adults with degenerative spinal conditions eligible to undergo a one to three-level MIS transforaminal lumbar interbody fusion (TLIF).
Six-month and 1-year radiographic fusion as determined by Suk criteria, postoperative opioid consumption as measured by intravenous milligram morphine equivalent, length of stay, and drug-related complications. Self-reported and functional measures include validated visual analog scale, short-form 12, and Oswestry Disability Index.
A double-blinded, randomized placebo-controlled, noninferiority trial of patients undergoing 1- to 3-level MIS TLIF was performed with bone morphogenetic protein (BMP). Patients were randomized to receive a 48-hour scheduled treatment of either intravenous ketorolac (15 mg every 6 hours) or saline in addition to a standardized pain regimen. The primary outcome was fusion. Secondary outcomes included 48-hour and total postoperative opioid use demonstrated as milligram morphine equivalence, pain scores, length of stay (LOS), and quality-of-life outcomes. Univariate analyses were performed. The present study provides results from a planned interim analysis.
Two hundred and forty-six patients were analyzed per protocol. Patient characteristics were comparable between the groups. There was no significant difference in 1-year fusion rates between the two treatments (p=.53). The difference in proportion of solid fusion between the ketorolac and placebo groups did not reach inferiority (p=.072, 95% confidence interval, -.07 to .21). There was a significant reduction in total/48-hour mean opioid consumption (p<.001) and LOS (p=.001) for the ketorolac group while demonstrating equivalent mean pain scores in 48 hours postoperative (p=.20). There was no significant difference in rates of perioperative complications.
Short-term use of low-dose ketorolac in patients who have undergone MIS TLIF with BMP demonstrated noninferior fusion rates. Ketorolac safely demonstrated a significant reduction in postoperative opioid use and LOS while maintaining equivalent postoperative pain control.
后路腰椎融合术后的疼痛控制仍然具有挑战性,通常需要大剂量的阿片类药物来缓解疼痛。由于存在假关节形成的风险,在脊柱融合术中使用酮咯酸受到限制。然而,最近的文献表明,短期低剂量使用酮咯酸并不会影响融合率。
我们旨在证明接受微创(MIS)后路腰椎椎间融合术的患者接受酮咯酸治疗后融合率无差异。此外,我们还旨在证明酮咯酸在术后即刻镇痛方面具有减少阿片类药物用量的作用。
研究设计/设置:这是一项前瞻性、随机、双盲、安慰剂对照试验。我们正在报告中期分析结果。
适合行单节段至三节段 MIS 经椎间孔腰椎体间融合术(TLIF)的成人退行性脊柱疾病患者。
术后 6 个月和 1 年的 Suk 标准影像学融合率、术后静脉注射吗啡等效物测量的阿片类药物消耗量、住院时间和与药物相关的并发症。自我报告和功能测量包括经过验证的视觉模拟量表、简短形式 12 项和 Oswestry 残疾指数。
对行 1 至 3 节段 MIS TLIF 术的患者进行了一项双盲、随机、安慰剂对照、非劣效性试验,其中使用了骨形态发生蛋白(BMP)。患者被随机分为两组,在标准镇痛方案的基础上,接受 48 小时计划治疗,分别接受静脉注射酮咯酸(15mg,每 6 小时一次)或生理盐水。主要结局为融合。次要结局包括术后 48 小时和总阿片类药物用量(以吗啡等效毫克数表示)、疼痛评分、住院时间(LOS)和生活质量结局。进行了单变量分析。本研究提供了计划中期分析的结果。
按方案分析了 246 例患者。两组患者的特征无显著差异。两组 1 年融合率无显著差异(p=.53)。酮咯酸组与安慰剂组之间固体融合比例的差异未达到劣效性(p=.072,95%置信区间,-.07 至.21)。酮咯酸组的总/48 小时平均阿片类药物消耗量(p<.001)和 LOS(p=.001)显著降低,而术后 48 小时平均疼痛评分相当(p=.20)。围手术期并发症发生率无显著差异。
在接受 MIS TLIF 术并使用 BMP 的患者中,短期使用低剂量酮咯酸可获得非劣效的融合率。酮咯酸安全地减少了术后阿片类药物的使用和 LOS,同时保持了等效的术后疼痛控制。
