Hersch Steven M, Schifitto Giovanni, Oakes David, Bredlau Amy-Lee, Meyers Catherine M, Nahin Richard, Rosas Herminia Diana
From the Department of Neurology (S.M.H., H.D.R.), Massachusetts General Hospital and Harvard Medical School, Boston; Departments of Neurology and Biostatistics (G.S., D.O.), University of Rochester Medical Center, NY; Department of Pediatrics (A.-L.B.), Medical University of South Carolina, Charleston; and NIH (C.M.M., R.N.), National Center for Complementary and Integrative Health, Bethesda, MD.
Neurology. 2017 Aug 8;89(6):594-601. doi: 10.1212/WNL.0000000000004209. Epub 2017 Jul 12.
To investigate whether creatine administration could slow progressive functional decline in adults with early symptoms of Huntington disease.
We conducted a multicenter, randomized, double-blind, placebo-controlled study of up to 40 g daily of creatine monohydrate in participants with stage I and II HD treated for up to 48 months. The primary outcome measure was the rate of change in total functional capacity (TFC) between baseline and end of follow-up. Secondary outcome measures included changes in additional clinical scores, tolerability, and quality of life. Safety was assessed by adverse events and laboratory studies.
At 46 sites in North America, Australia, and New Zealand, 553 participants were randomized to creatine (275) or placebo (278). The trial was designed to enroll 650 patients, but was halted for futility after the first interim analysis. The estimated rates of decline in the primary outcome measure (TFC) were 0.82 points per year for participants on creatine, 0.70 points per year for participants on placebo, favoring placebo (nominal 95% confidence limits -0.11 to 0.35). Adverse events, mainly gastrointestinal, were significantly more common in participants on creatine. Serious adverse events, including deaths, were more frequent in the placebo group. Subgroup analysis suggested that men and women may respond differently to creatine treatment.
Our data do not support the use of creatine treatment for delaying functional decline in early manifest HD.
NCT00712426.
This study provides Class II evidence that for patients with early symptomatic HD, creatine monohydrate is not beneficial for slowing functional decline.
研究补充肌酸是否能减缓患有亨廷顿病早期症状的成年人的功能进行性衰退。
我们开展了一项多中心、随机、双盲、安慰剂对照研究,对处于Ⅰ期和Ⅱ期的亨廷顿病患者每日服用高达40克的一水肌酸,治疗长达48个月。主要结局指标是基线至随访结束时总功能能力(TFC)的变化率。次要结局指标包括其他临床评分的变化、耐受性和生活质量。通过不良事件和实验室检查评估安全性。
在北美、澳大利亚和新西兰的46个地点,553名参与者被随机分为肌酸组(275人)或安慰剂组(278人)。该试验原计划招募650名患者,但在首次中期分析后因无效而停止。主要结局指标(TFC)的估计衰退率为:服用肌酸的参与者每年0.82分,服用安慰剂的参与者每年0.70分,安慰剂组更优(名义95%置信区间为-0.11至0.35)。不良事件主要是胃肠道方面的,在服用肌酸的参与者中明显更常见。严重不良事件,包括死亡,在安慰剂组中更频繁。亚组分析表明,男性和女性对肌酸治疗的反应可能不同。
我们的数据不支持使用肌酸治疗来延缓早期显性亨廷顿病的功能衰退。
NCT00712426。
本研究提供了Ⅱ级证据,表明对于早期有症状的亨廷顿病患者,一水肌酸对减缓功能衰退无益处。
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