Chen Christopher, Katayama Sadao, Lee Jae-Hong, Lee Jun-Young, Nakagawa Masaki, Torii Kentaro, Ogawa Tomoo, Dash Amitabh, Irizarry Michael, Dhadda Shobha, Kanekiyo Michio, Hersch Steve, Iwatsubo Takeshi
Memory Aging and Cognition Center, Department of Pharmacology, Yong Loo Lin School of Medicine, National University of Singapore, Singapore.
Katayama Medical Clinic, Kurashiki, Japan.
J Prev Alzheimers Dis. 2025 May;12(5):100160. doi: 10.1016/j.tjpad.2025.100160. Epub 2025 Apr 5.
Across Asia, Alzheimer's disease prevalence is expected to rise dramatically due to, among other factors, rapidly aging populations. Alzheimer's disease pathology is triggered by the accumulation of soluble and insoluble aggregated Aβ peptides (oligomers, protofibrils, and fibrils). Lecanemab is a recently approved humanized IgG1 monoclonal antibody that preferentially targets soluble aggregated Aβ species (oligomers, protofibrils), with activity at insoluble fibrils. In the recent 18-month phase 3 Clarity AD study, lecanemab demonstrated a consistent slowing of decline in clinical (global, cognitive, functional, and quality of life) outcomes, and reduction in brain amyloid in early Alzheimer's disease. Lecanemab was well tolerated in Clarity AD, with an increase in incidence of infusion related reactions and amyloid-related imaging abnormalities (ARIA) versus placebo.
The objective of this manuscript is to present the results for the Asian region population of Clarity AD.
The core Clarity AD study was an 18-month, multicenter, double-blind, placebo-controlled, parallel-group study.
Academic and clinical centers in Asia PARTICIPANTS: A total of 294 individuals with early Alzheimer's disease (i.e., mild cognitive impairment or mild Alzheimer's disease).
Eligible patients were randomized across 2 treatment groups (placebo and lecanemab 10 mg/kg biweekly) according to a fixed 1:1 schedule.
The primary efficacy endpoint in the core study was change in the Clinical Dementia Rating-Sum-of-Boxes (CDR-SB) from baseline at 18 months. Key secondary endpoints included change from baseline at 18 months in amyloid PET Centiloids (in patients participating in the amyloid PET sub-study), AD COMposite Score (ADCOMS) and AD Assessment Scale-Cognitive Subscale 14 (ADAS-Cog14). Safety was monitored throughout the study in a blinded manner by the sponsor and in an unblinded manner by an independent data safety monitoring committee.
Of the total of 1795 subjects randomized in Clarity AD, 294 subjects were in the Asian region (Japan:152; Korea:129; Singapore:13). The efficacy of lecanemab was consistent with the overall population. For the primary endpoint, there was a slowing of decline with lecanemab in the CDR-SB at 18 months compared to placebo in the Asian region (adjusted mean difference: -0.349; 95 % confidence intervals: -0.773, 0.076; 24 % slowing of decline). Results for the secondary efficacy endpoints also favored lecanemab versus placebo in Asians. Lecanemab was well tolerated in Asian subjects, with a safety profile in Asian subjects similar to the overall Clarity AD population. The most common adverse events of special interest were ARIA-H (lecanemab:14.4 %; placebo:16.2 %), ARIA-E (lecanemab:6.2 %; placebo:1.4 %), and infusion-related reactions (lecanemab:12.3 %; placebo:1.4 %). Incidence of adverse events leading to study drug dose interruption or withdrawal, infusion-related reactions, ARIA-E and ARIA-H was lower for the lecanemab treated group in the Asian region relative to the overall Clarity AD population. Results from quality of life and biomarker assessments in the Asia region were also generally similar to the overall Clarity AD population.
In the Clarity AD Asian region cohort, the overall efficacy, biomarker changes and safety profile of lecanemab were consistent with the overall population, with a favorable risk-benefit profile and manageable risks. ARIA events and infusion-related reactions occurred less commonly with lecanemab in the Asian region subgroup than the overall population.
在亚洲,由于人口快速老龄化等因素,阿尔茨海默病的患病率预计将急剧上升。阿尔茨海默病的病理变化是由可溶性和不溶性聚集的Aβ肽(寡聚体、原纤维和纤维)的积累引发的。仑卡奈单抗是一种最近获批的人源化IgG1单克隆抗体,它优先靶向可溶性聚集的Aβ物种(寡聚体、原纤维),对不溶性纤维也有活性。在最近为期18个月的3期Clarity AD研究中,仑卡奈单抗在早期阿尔茨海默病中显示出临床(整体、认知、功能和生活质量)结局下降持续减缓,以及脑淀粉样蛋白减少。在Clarity AD研究中,仑卡奈单抗耐受性良好,与安慰剂相比,输液相关反应和淀粉样蛋白相关成像异常(ARIA)的发生率有所增加。
本手稿的目的是展示Clarity AD研究中亚洲地区人群的结果。
核心Clarity AD研究是一项为期18个月的多中心、双盲、安慰剂对照、平行组研究。
亚洲的学术和临床中心
共有294例早期阿尔茨海默病患者(即轻度认知障碍或轻度阿尔茨海默病)。
符合条件的患者按照固定的1:1方案随机分为2个治疗组(安慰剂和每两周一次10 mg/kg的仑卡奈单抗)。
核心研究的主要疗效终点是18个月时临床痴呆评定量表总和(CDR-SB)相对于基线的变化。关键次要终点包括18个月时淀粉样蛋白PET百分位数(参与淀粉样蛋白PET子研究的患者)相对于基线的变化、AD综合评分(ADCOMS)和AD评估量表-认知子量表14(ADAS-Cog14)。在整个研究过程中,申办者以盲法监测安全性,独立数据安全监测委员会以非盲法监测安全性。
在Clarity AD研究中随机分组的1795名受试者中,294名受试者来自亚洲地区(日本:152名;韩国:129名;新加坡:13名)。仑卡奈单抗的疗效与总体人群一致。对于主要终点,在亚洲地区,与安慰剂相比,18个月时仑卡奈单抗治疗组的CDR-SB下降减缓(调整后平均差异:-0.349;95%置信区间:-0.773,0.076;下降减缓24%)。次要疗效终点的结果在亚洲人中也有利于仑卡奈单抗而非安慰剂。仑卡奈单抗在亚洲受试者中耐受性良好,亚洲受试者的安全性概况与Clarity AD总体人群相似。特别关注的最常见不良事件是ARIA-H(仑卡奈单抗:14.4%;安慰剂:16.2%)、ARIA-E(仑卡奈单抗:6.2%;安慰剂:1.4%)和输液相关反应(仑卡奈单抗:12.3%;安慰剂:1.4%)。亚洲地区仑卡奈单抗治疗组导致研究药物剂量中断或停药、输液相关反应、ARIA-E和ARIA-H的不良事件发生率低于Clarity AD总体人群。亚洲地区生活质量和生物标志物评估的结果也与Clarity AD总体人群总体相似。
在Clarity AD亚洲地区队列中,仑卡奈单抗的总体疗效、生物标志物变化和安全性概况与总体人群一致,具有良好的风险效益概况和可控风险。在亚洲地区亚组中,仑卡奈单抗引起的ARIA事件和输液相关反应比总体人群更少见。
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