Orthopedics Department B, Tel Aviv Sourasky Medical Center.
Pain Med. 2010 Mar;11(3):356-68. doi: 10.1111/j.1526-4637.2010.00808.x.
Objective. Agmatine, decarboxylated arginine, was shown in preclinical studies to exert efficacious neuroprotection by interacting with multiple molecular targets. This study was designed to ascertain safety and efficacy of dietary agmatine sulfate in herniated lumbar disc-associated radiculopathy. Study Design. First, an open-label dose escalation study was performed to assess the safety and side-effects of agmatine sulfate. In the follow-up study, participants diagnosed with herniated lumbar disc-associated radiculopathy were randomly assigned to receive either placebo or agmatine sulfate in a double-blind fashion. Methods. Participants in the first study were recruited consecutively into four cohorts who took the following escalating regimens: 1.335 g/day agmatine sulfate for 10 days, 2.670 g/day for 10 days, 3.560 g/day for 10 days, and 3.560 g/day for 21 days. Participants in the follow-up study were assigned to receive either placebo or agmatine sulfate, 2.670 g/day for 14 days. Primary outcome measures were pain using the visual analog scale, the McGill pain questionnaire and the Oswestry disability index, sensorimotor deficits, and health-related quality of life using the 36-item short form (SF-36) questionnaire. Secondary outcomes included other treatment options, and safety and tolerability assessment. Results. Safety parameters were within normal values in all participants of the first study. Three participants in the highest dose cohort had mild-to-moderate diarrhea and mild nausea during treatment, which disappeared upon treatment cessation. No other events were observed. In the follow-up study, 51 participants were randomly enrolled in the agmatine group and 48 in the placebo. Continuous improvement of symptoms occurred in both groups, but was more pronounced in the agmatine (analyzed n = 31) as compared with the placebo group (n = 30). Expressed as percent of baseline values, significantly enhanced improvement in average pain measures and in quality of life scores occurred after treatment in the agmatine group (26.7% and 70.8%, respectively) as compared with placebo (6.0% [P </= 0.05] and 20.0% [P </= 0.05], respectively). No treatment-related adverse events were noted. Conclusions. Dietary agmatine sulfate is safe and efficacious treatment for alleviating pain and improving quality of life in lumbar disc-associated radiculopathy. Study Registration. ClinicalTrials.gov Protocol Registration System Identifier: NCT00405041.
精氨酸脱羧产物胍丁胺通过与多种分子靶点相互作用,在临床前研究中显示出有效的神经保护作用。本研究旨在确定硫酸胍丁胺在腰椎间盘突出症相关神经根病中的安全性和疗效。
首先,进行了一项开放性标签剂量递增研究,以评估硫酸胍丁胺的安全性和副作用。在后续研究中,将诊断为腰椎间盘突出症相关神经根病的参与者随机分为安慰剂组或硫酸胍丁胺组进行双盲治疗。
第一项研究中,连续招募了四组参与者,他们服用以下递增方案的硫酸胍丁胺:1.335 g/天,持续 10 天;2.670 g/天,持续 10 天;3.560 g/天,持续 10 天;3.560 g/天,持续 21 天。后续研究中的参与者被分配接受安慰剂或硫酸胍丁胺,剂量为 2.670 g/天,持续 14 天。主要观察指标为使用视觉模拟评分法、麦吉尔疼痛问卷和 Oswestry 残疾指数评估的疼痛,使用 36 项简明健康状况调查问卷评估的感觉运动缺陷和健康相关生活质量。次要结局指标包括其他治疗选择以及安全性和耐受性评估。
第一项研究中所有参与者的安全性参数均在正常范围内。高剂量组的 3 名参与者在治疗期间出现轻度至中度腹泻和轻度恶心,但停药后消失。未观察到其他事件。在后续研究中,51 名参与者被随机分配到胍丁胺组,48 名参与者被分配到安慰剂组。两组症状均持续改善,但胍丁胺组(分析 n = 31)的改善更为明显,而安慰剂组(n = 30)的改善不明显。与安慰剂组相比,接受治疗后,胍丁胺组平均疼痛测量和生活质量评分的改善幅度明显更大,分别为 26.7%和 70.8%(分别为[P </= 0.05]和[P </= 0.05])。未观察到与治疗相关的不良事件。
膳食硫酸胍丁胺是治疗腰椎间盘突出症相关神经根病的安全有效方法,可缓解疼痛,提高生活质量。
ClinicalTrials.gov 协议注册系统标识符:NCT00405041。
