Schneider Lon S, Thomas Ronald G, Hendrix Suzanne, Rissman Robert A, Brewer James B, Salmon David P, Oltersdorf Tilman, Okuda Tomohiro, Feldman Howard H
Keck School of Medicine of the University of Southern California, Los Angeles.
Department of Neurosciences, University of California San Diego School of Medicine.
JAMA Neurol. 2019 Nov 1;76(11):1330-1339. doi: 10.1001/jamaneurol.2019.1868.
Edonerpic maleate (T-817MA) protects against Aβ40-induced neurotoxic effects and memory deficits, promotes neurite outgrowth, and preserves hippocampal synapses and spatial memory in tau transgenic mice. These effects may be mediated via sigma-1 receptor activation, delivery of synaptic AMPA receptors, or modulation of microglial function and may benefit patients with Alzheimer disease.
To assess the efficacy, safety, and tolerability of edonerpic for patients with mild to moderate Alzheimer disease.
DESIGN, SETTING, AND PARTICIPANTS: Randomized, double-blind, placebo-controlled, parallel-group, phase 2 clinical trial conducted over 52 weeks from June 2, 2014, to December 14, 2016, at 52 US clinical and academic centers. Of 822 outpatients screened, 484 met the following criteria and were randomly assigned to treatment: 55 to 85 years of age, probable Alzheimer disease, Mini-Mental State Examination scores from 12 to 22, and taking stable doses of donepezil or rivastigmine with or without memantine.
Random assignment (1:1:1 allocation) to placebo or 224 mg or 448 mg of edonerpic maleate, once per day.
Coprimary outcomes were scores on the Alzheimer Disease Assessment Scale-Cognitive Subscale (ADAS-cog) and Alzheimer's Disease Cooperative Study-Clinical Impression of Change (ADCS-CGIC) at week 52. Biomarkers were brain, lateral ventricular, and hippocampal volumes, as determined on magnetic resonance imaging, and cerebrospinal fluid Aβ40, Aβ42, total tau, and phospho-tau181. The primary efficacy analysis was performed on the coprimary end points for the modified intention-to-treat population.
Of 482 participants in the safety population, 140 of 158 participants (88.6%) assigned to placebo, 117 of 166 participants (70.5%) to 224 mg of edonerpic maleate, and 120 of 158 participants (76.0%) to 448 mg of edonerpic maleate completed the trial. The mean ADAS-cog score change at week 52 was 7.91 for the placebo group, 7.45 for the 224-mg group, and 7.08 for the 448-mg group. Mean differences from placebo were -0.47 (95% CI, -2.36 to 1.43; P = .63) for the 224-mg group and -0.84 (95% CI, -2.75 to 1.08; P = .39) for the 448-mg group. Mean ADCS-CGIC scores were 5.22 for the placebo group, 5.24 for the 224-mg group, and 5.25 for the 448-mg group, with mean differences from placebo of 0.03 (95% CI, -0.20 to 0.25; P = .81) for the 224-mg group and 0.04 (95% CI, -0.19 to 0.26; P = .76) for the 448-mg group. In the safety population, a total of 7 of 158 participants (4.4%) in the placebo group, 23 of 166 participants (13.9%) in the 224-mg group, and 23 of 158 participants (14.6%) in the 448-mg group discontinued because of adverse events. The most frequent adverse events were diarrhea and vomiting.
Edonerpic maleate appeared to be safe and tolerable, with expected gastrointestinal symptoms occurring early but without evidence for a clinical effect among patients with mild to moderate Alzheimer disease.
ClinicalTrials.gov identifier: NCT02079909.
马来酸依度那匹(T - 817MA)可预防Aβ40诱导的神经毒性作用和记忆缺陷,促进神经突生长,并在tau转基因小鼠中保留海马突触和空间记忆。这些作用可能通过sigma - 1受体激活、突触AMPA受体的传递或小胶质细胞功能的调节介导,可能使阿尔茨海默病患者受益。
评估马来酸依度那匹对轻度至中度阿尔茨海默病患者的疗效、安全性和耐受性。
设计、地点和参与者:2014年6月2日至2016年12月14日在美国52个临床和学术中心进行的随机、双盲、安慰剂对照、平行组2期临床试验。在822名筛查的门诊患者中,484名符合以下标准并被随机分配接受治疗:年龄55至85岁,可能患有阿尔茨海默病,简易精神状态检查表评分12至22,且正在服用稳定剂量的多奈哌齐或利伐斯的明,可加用或不加用美金刚。
随机分配(1:1:1分配)接受安慰剂或224毫克或448毫克马来酸依度那匹,每日一次。
共同主要结局是第52周时阿尔茨海默病评估量表认知子量表(ADAS - cog)和阿尔茨海默病协作研究 - 变化的临床印象(ADCS - CGIC)的评分。生物标志物包括通过磁共振成像测定的脑、侧脑室和海马体积,以及脑脊液Aβ40、Aβ42、总tau和磷酸化tau181。对改良意向性治疗人群的共同主要终点进行主要疗效分析。
在安全人群的482名参与者中,分配到安慰剂组的158名参与者中有140名(88.6%)、分配到224毫克马来酸依度那匹组的166名参与者中有117名(70.5%)、分配到448毫克马来酸依度那匹组的158名参与者中有120名(76.0%)完成了试验。安慰剂组第52周时ADAS - cog评分的平均变化为7.91,224毫克组为7.45,448毫克组为7.08。224毫克组与安慰剂组的平均差异为 - 0.47(95%置信区间, - 2.36至1.43;P = 0.63),448毫克组为 - 0.84(95%置信区间, - 2.75至1.08;P = 0.39)。安慰剂组的平均ADCS - CGIC评分为5.22,2