Selection design phase II trial of high dosages of tamoxifen and creatine in amyotrophic lateral sclerosis

IF 2.5 4区 医学 Q2 CLINICAL NEUROLOGY
Suma Babu, E. Macklin, K. Jackson, Elizabeth Simpson, K. Mahoney, Hong Yu, Jason Walker, Z. Simmons, W. David, P. Barkhaus, L. Simionescu, M. Dimachkie, A. Pestronk, J. Salameh, M. Weiss, B. Brooks, D. Schoenfeld, J. Shefner, Swati Aggarwal, M. Cudkowicz, N. Atassi
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引用次数: 10

Abstract

Abstract Objective: To conduct a phase-II trial using a ranking and selection paradigm where multiple treatments are compared with limited sample size and the best is chosen for a subsequent efficacy trial versus placebo. This strategy can find an effective treatment faster than traditional strategy of conducting larger trials against placebo. Methods: Sixty amyotrophic lateral sclerosis (ALS) participants were randomized 1:1:1 to creatine 30 g/day (CRE), tamoxifen 40 mg/day (T40), or tamoxifen 80 mg/day (T80), with matching placebo. The primary outcome was 38-week change in ALS Functional Rating Scale-Revised (ALSFRS-R), analyzed in a repeated-measures ANOVA. Secondary outcomes included slow vital capacity (SVC), quantitative muscle strength, early drug discontinuation (EDD), adverse events (AEs), and survival. Results: CRE participants experienced higher rates of drug-related AEs (82% vs. 43% T40, 47% T80) and EDD (50% vs. 24% T40, 29% T80). T80 participants experienced slower adjusted mean decline in ALSFRS-R in points/month (–0.80 vs. –0.84 T40, –0.85 CRE) and quantitative muscle strength but not in SVC and higher rates of mortality. Conclusion: Efficacy of T80 ranked numerically superior to CRE and T40 with respect to ALSFRS-R decline. Following the selection paradigm, T80 would be chosen to test against placebo. The approach was not designed to distinguish among treatments that are nearly equally effective or ineffective. If treatments are equivalent, then under the paradigm, it does not matter which treatment is selected. Newer approaches for increasing trial efficiency, including an adaptive platform trial design, may mitigate limitations of the selection design.
高剂量他莫昔芬和肌酸治疗肌萎缩侧索硬化症的选择设计II期试验
摘要目的:使用排名和选择范式进行II期试验,在有限的样本量下比较多种治疗方法,并在随后的疗效试验中选择最佳治疗方法与安慰剂进行比较。这种策略可以比传统的针对安慰剂进行大规模试验的策略更快地找到有效的治疗方法。方法:60名肌萎缩侧索硬化症(ALS)参与者以1:1:1的比例随机接受肌酸30 g/天(CRE),他莫昔芬40 mg/天(T40)或他莫昔芬80 mg/天(T80),与匹配的安慰剂。主要结果是ALS功能评定量表修订版(ALSFRS-R)38周的变化,通过重复测量方差分析进行分析。次要结果包括缓慢肺活量(SVC)、定量肌肉力量、早期停药(EDD)、不良事件(AE)和生存率。结果:CRE参与者经历了更高的药物相关AE发生率(82%对43%的T40,47%的T80)和EDD发生率(50%对24%的T40和29%的T90)。T80参与者的ALSFRS-R的调整后平均下降速度较慢,以点/月为单位(-0.80 vs.-0.84 T40,-0.85 CRE),肌肉力量定量下降,但SVC和死亡率较高。结论:在ALSFRS-R下降方面,T80的疗效在数量上优于CRE和T40。按照选择范式,T80将被选择与安慰剂进行测试。该方法并不是为了区分几乎同等有效或无效的治疗方法。如果治疗是等效的,那么在范式下,选择哪种治疗并不重要。提高试验效率的新方法,包括自适应平台试验设计,可以减轻选择设计的局限性。
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来源期刊
CiteScore
5.40
自引率
10.70%
发文量
64
期刊介绍: Amyotrophic Lateral Sclerosis and Frontotemporal Degeneration is an exciting new initiative. It represents a timely expansion of the journal Amyotrophic Lateral Sclerosis in response to the clinical, imaging pathological and genetic overlap between ALS and frontotemporal dementia. The expanded journal provides outstanding coverage of research in a wide range of issues related to motor neuron diseases, especially ALS (Lou Gehrig’s disease) and cognitive decline associated with frontotemporal degeneration. The journal also covers related disorders of the neuroaxis when relevant to these core conditions.
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