早期阿尔茨海默病中的lecanemab
Lecanemab in Early Alzheimer's Disease.
作者信息
van Dyck Christopher H, Swanson Chad J, Aisen Paul, Bateman Randall J, Chen Christopher, Gee Michelle, Kanekiyo Michio, Li David, Reyderman Larisa, Cohen Sharon, Froelich Lutz, Katayama Sadao, Sabbagh Marwan, Vellas Bruno, Watson David, Dhadda Shobha, Irizarry Michael, Kramer Lynn D, Iwatsubo Takeshi
机构信息
From the Alzheimer's Disease Research Unit, Yale School of Medicine, New Haven, CT (C.H.D.); Eisai, Nutley, NJ (C.J.S., M.K., D.L., L.R., S.D., M.I., L.D.K.); the Alzheimer's Therapeutic Research Institute, University of Southern California, San Diego (P.A.); Washington University School of Medicine in St. Louis, St. Louis (R.B.); the Memory, Aging, and Cognition Center, Department of Pharmacology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore (C.C.); Eisai, Hatfield, United Kingdom (M.G.); Toronto Memory Program, Toronto (S.C.); Medical Faculty Mannheim, University of Heidelberg, Central Institute of Mental Health, Mannheim, Germany (L.F.); Katayama Medical Clinic, Okayama (S.K.), and the Department of Neuropathology, Graduate School of Medicine, University of Tokyo, and the National Center of Neurology and Psychiatry, Tokyo (T.I.) - all in Japan; Barrow Neurological Institute, Phoenix, AZ (M.S.); Toulouse Gerontopole University Hospital, Université Paul Sabatier, INSERM Unité 1295, Toulouse, France (B.V.); and Alzheimer's Research and Treatment Center, Wellington, FL (D.W.).
出版信息
N Engl J Med. 2023 Jan 5;388(1):9-21. doi: 10.1056/NEJMoa2212948. Epub 2022 Nov 29.
BACKGROUND
The accumulation of soluble and insoluble aggregated amyloid-beta (Aβ) may initiate or potentiate pathologic processes in Alzheimer's disease. Lecanemab, a humanized IgG1 monoclonal antibody that binds with high affinity to Aβ soluble protofibrils, is being tested in persons with early Alzheimer's disease.
METHODS
We conducted an 18-month, multicenter, double-blind, phase 3 trial involving persons 50 to 90 years of age with early Alzheimer's disease (mild cognitive impairment or mild dementia due to Alzheimer's disease) with evidence of amyloid on positron-emission tomography (PET) or by cerebrospinal fluid testing. Participants were randomly assigned in a 1:1 ratio to receive intravenous lecanemab (10 mg per kilogram of body weight every 2 weeks) or placebo. The primary end point was the change from baseline at 18 months in the score on the Clinical Dementia Rating-Sum of Boxes (CDR-SB; range, 0 to 18, with higher scores indicating greater impairment). Key secondary end points were the change in amyloid burden on PET, the score on the 14-item cognitive subscale of the Alzheimer's Disease Assessment Scale (ADAS-cog14; range, 0 to 90; higher scores indicate greater impairment), the Alzheimer's Disease Composite Score (ADCOMS; range, 0 to 1.97; higher scores indicate greater impairment), and the score on the Alzheimer's Disease Cooperative Study-Activities of Daily Living Scale for Mild Cognitive Impairment (ADCS-MCI-ADL; range, 0 to 53; lower scores indicate greater impairment).
RESULTS
A total of 1795 participants were enrolled, with 898 assigned to receive lecanemab and 897 to receive placebo. The mean CDR-SB score at baseline was approximately 3.2 in both groups. The adjusted least-squares mean change from baseline at 18 months was 1.21 with lecanemab and 1.66 with placebo (difference, -0.45; 95% confidence interval [CI], -0.67 to -0.23; P<0.001). In a substudy involving 698 participants, there were greater reductions in brain amyloid burden with lecanemab than with placebo (difference, -59.1 centiloids; 95% CI, -62.6 to -55.6). Other mean differences between the two groups in the change from baseline favoring lecanemab were as follows: for the ADAS-cog14 score, -1.44 (95% CI, -2.27 to -0.61; P<0.001); for the ADCOMS, -0.050 (95% CI, -0.074 to -0.027; P<0.001); and for the ADCS-MCI-ADL score, 2.0 (95% CI, 1.2 to 2.8; P<0.001). Lecanemab resulted in infusion-related reactions in 26.4% of the participants and amyloid-related imaging abnormalities with edema or effusions in 12.6%.
CONCLUSIONS
Lecanemab reduced markers of amyloid in early Alzheimer's disease and resulted in moderately less decline on measures of cognition and function than placebo at 18 months but was associated with adverse events. Longer trials are warranted to determine the efficacy and safety of lecanemab in early Alzheimer's disease. (Funded by Eisai and Biogen; Clarity AD ClinicalTrials.gov number, NCT03887455.).
背景
可溶性和不溶性聚集的β-淀粉样蛋白(Aβ)的积累可能引发或加剧阿尔茨海默病的病理过程。Lecanemab是一种人源化IgG1单克隆抗体,可与Aβ可溶性原纤维高亲和力结合,目前正在早期阿尔茨海默病患者中进行试验。
方法
我们进行了一项为期18个月的多中心、双盲3期试验,纳入年龄在50至90岁之间的早期阿尔茨海默病患者(因阿尔茨海默病导致的轻度认知障碍或轻度痴呆),这些患者通过正电子发射断层扫描(PET)或脑脊液检测有淀粉样蛋白证据。参与者按1:1的比例随机分配,接受静脉注射Lecanemab(每2周每公斤体重10毫克)或安慰剂。主要终点是18个月时临床痴呆评定量表总和(CDR-SB;范围为0至18,分数越高表明损害越严重)得分相对于基线的变化。关键次要终点是PET上淀粉样蛋白负荷的变化、阿尔茨海默病评估量表14项认知子量表(ADAS-cog14;范围为0至90;分数越高表明损害越严重)得分、阿尔茨海默病综合评分(ADCOMS;范围为0至1.97;分数越高表明损害越严重)以及阿尔茨海默病合作研究-轻度认知障碍日常生活活动量表(ADCS-MCI-ADL;范围为0至53;分数越低表明损害越严重)得分。
结果
共纳入1795名参与者,其中898名被分配接受Lecanemab,897名接受安慰剂。两组在基线时的平均CDR-SB得分约为3.2。18个月时,Lecanemab组相对于基线的调整后最小二乘均值变化为1.21,安慰剂组为1.66(差异为-0.45;95%置信区间[CI]为-0.67至-0.23;P<0.001)。在一项涉及698名参与者的亚研究中,Lecanemab组脑淀粉样蛋白负荷的降低幅度大于安慰剂组(差异为-59.1个百分位数;95%CI为-62.6至-55.6)。两组之间相对于基线变化的其他平均差异有利于Lecanemab的情况如下:ADAS-cog14得分,-1.44(95%CI为-2.27至-0.61;P<0.001);ADCOMS得分,-0.050(95%CI为-0.074至-0.027;P<0.001);ADCS-MCI-ADL得分,2.0(95%CI为1.2至2.8;P<0.001)。Lecanemab导致26.4%的参与者出现输液相关反应,12.6%的参与者出现与淀粉样蛋白相关的影像学异常伴水肿或积液。
结论
Lecanemab降低了早期阿尔茨海默病患者的淀粉样蛋白标志物,在18个月时认知和功能测量指标上的下降程度比安慰剂适度减轻,但与不良事件相关。有必要进行更长时间的试验来确定Lecanemab在早期阿尔茨海默病中的疗效和安全性。(由卫材和百健资助;Clarity AD临床试验注册号,NCT03887455。)
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