阿尔茨海默病中RAGE-Aβ相互作用抑制剂的临床试验。
Clinical trial of an inhibitor of RAGE-Aβ interactions in Alzheimer disease.
作者信息
Galasko Douglas, Bell Joanne, Mancuso Jessica Y, Kupiec James W, Sabbagh Marwan N, van Dyck Christopher, Thomas Ronald G, Aisen Paul S
机构信息
From the Department of Neurosciences (D.G., R.G.T., P.S.A.), University of California, San Diego; Pfizer Global Research & Development (J.B., J.Y.M., J.W.K.), Cambridge, MA; Banner Sun Health Research Institute (M.N.S.), Sun City; University of Arizona (M.N.S.), Tucson; and the Department of Psychiatry (C.v.D.), Yale University, New Haven, CT.
出版信息
Neurology. 2014 Apr 29;82(17):1536-42. doi: 10.1212/WNL.0000000000000364. Epub 2014 Apr 2.
OBJECTIVE
To examine safety, tolerability, and efficacy of PF-04494700, an inhibitor of the receptor for advanced glycation end products (RAGE), in mild to moderate Alzheimer disease (AD).
METHODS
Double-blind, placebo-controlled trial at 40 academic centers (United States). Subjects with AD and Mini-Mental State Examination score 14-26 were randomized to PF-04494700 60 mg/day × 6 days, then 20 mg daily (high dose); 15 mg/day × 6 days, then 5 mg daily (low dose); or placebo, for 18 months. Clinical and laboratory measures were used to evaluate safety and tolerability. The primary efficacy measure was the Alzheimer's Disease Assessment Scale-cognitive (ADAS-cog). Secondary measures assessed clinical stage, function, behavior, MRI, and CSF biomarkers.
RESULTS
A total of 399 subjects were randomized. In a prespecified interim analysis, when 50% of subjects had completed the 6-month visit, the high dose was associated with confusion, falls, and greater ADAS-cog decline and was discontinued. A second prespecified analysis compared low-dose and placebo groups for futility and safety approximately 12 months after all subjects were randomized. This analysis met criteria for futility, and treatment was discontinued. There were no safety concerns in the low-dose group. Analyses including post-futility data showed decreased decline on the ADAS-cog in the low-dose group at month 18. Other clinical and biomarker measures showed no differences between low-dose treatment and placebo.
CONCLUSIONS
PF-04494700 at 20 mg/d was associated with increased adverse events and cognitive decline. At 5 mg/d, PF-04494700 had a good safety profile. A potential benefit for this low dose on the ADAS-cog is not conclusive, because of high dropout and discontinuation rates subsequent to the interim analyses.
CLASSIFICATION OF EVIDENCE
This study provides Class I evidence that in patients with AD high-dose PF-04494700 increased cognitive decline at 6 months and Class IV evidence that low-dose PF-04494700 slowed cognitive decline at 18 months.
目的
研究晚期糖基化终末产物受体(RAGE)抑制剂PF-04494700在轻度至中度阿尔茨海默病(AD)中的安全性、耐受性和疗效。
方法
在美国40个学术中心进行的双盲、安慰剂对照试验。AD患者且简易精神状态检查表评分14 - 26分被随机分为PF-04494700 60毫克/天×6天,然后20毫克/天(高剂量);15毫克/天×6天,然后5毫克/天(低剂量);或安慰剂组,为期18个月。采用临床和实验室指标评估安全性和耐受性。主要疗效指标是阿尔茨海默病评估量表认知部分(ADAS-cog)。次要指标评估临床分期、功能、行为、磁共振成像(MRI)和脑脊液生物标志物。
结果
共399名受试者被随机分组。在一项预先设定的中期分析中,当50%的受试者完成6个月访视时,高剂量组出现意识混乱、跌倒以及ADAS-cog下降更明显,因此停药。在所有受试者随机分组约12个月后进行的第二项预先设定分析比较了低剂量组和安慰剂组的无效性和安全性。该分析符合无效标准,治疗停止。低剂量组无安全性问题。包括无效性分析后数据的分析显示,低剂量组在第18个月时ADAS-cog下降减缓。其他临床和生物标志物指标显示低剂量治疗组与安慰剂组之间无差异。
结论
20毫克/天的PF-04494700与不良事件增加和认知功能下降相关。5毫克/天的PF-04494700具有良好的安全性。由于中期分析后高脱落率和停药率,该低剂量对ADAS-cog的潜在益处尚无定论。
证据分级
本研究提供I级证据表明,在AD患者中,高剂量PF-04494700在6个月时增加认知功能下降;提供IV级证据表明,低剂量PF-04494700在18个月时减缓认知功能下降。
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