Zimmer Jennifer A, Shcherbinin Sergey, Devous Michael D, Bragg Sonja M, Selzler Katherine J, Wessels Alette M, Shering Craig, Mullen Jamie, Landry John, Andersen Scott W, Downing AnnCatherine M, Fleisher Adam S, Svaldi Diana Otero, Sims John R
Eli Lilly and Company Indianapolis Indiana USA.
AstraZeneca, Neuroscience Biopharmaceuticals R&D Boston Massachusetts USA.
Alzheimers Dement (N Y). 2021 Feb 14;7(1):e12123. doi: 10.1002/trc2.12123. eCollection 2021.
Lanabecestat, a beta-site amyloid precursor protein-cleaving enzyme 1 (BACE1) inhibitor, was investigated as a potential Alzheimer's disease (AD)-modifying treatment. As previously reported, amyloid beta (Aβ) neuritic plaque burden reduction did not result in clinical benefit. Lanabecestat's effects on neuroimaging biomarkers and correlations between neuroimaging biomarkers and efficacy measures are reported.
AMARANTH and DAYBREAK-ALZ were 104- and 78-week, multicenter, randomized, double-blind, placebo-controlled studies of lanabecestat in early symptomatic AD (AMARANTH) and mild AD dementia (DAYBREAK-ALZ). Patients randomly (1:1:1) received placebo, lanabecestat 20 mg, or lanabecestat 50 mg daily (AMARANTH, n = 2218; DAYBREAK-ALZ, n = 1722). Florbetapir positron emission tomography (PET), fluorodeoxyglucose (FDG) PET, flortaucipir PET, and volumetric magnetic resonance imaging (MRI) were used to measure Aβ neuritic plaque burden, cerebral metabolism, aggregated tau neurofibrillary tangles, and brain volume, respectively. Additionally, florbetapir perfusion scans were performed in DAYBREAK-ALZ. Efficacy measures included 13-item Alzheimer's Disease Assessment Scale-Cognitive Subscale, Alzheimer's Disease Cooperative Study Activities of Daily Living Inventory, Clinical Dementia Rating-Sum of Boxes, Functional Activities Questionnaire, and Mini-Mental State Examination. These studies stopped early due to futility.
Despite previously observed annualized reduction in Aβ neuritic plaque burden, there were no treatment differences in annualized change of aggregated tau neurofibrillary tangle burden (AMARANTH, n = 284; DAYBREAK-ALZ, n = 70), cerebral metabolism (AMARANTH, n = 260; DAYBREAK-ALZ, n = 38) and perfusion (DAYBREAK-ALZ, n = 213). Greater brain volume reduction (AMARANTH, n = 1697 [whole brain]; DAYBREAK-ALZ, n = 650 [whole brain]) occurred on lanabecestat compared to placebo. Higher baseline aggregated tau neurofibrillary tangle burden, lower cerebral metabolism, and lower brain volumes correlated with poorer baseline efficacy scores and greater clinical worsening. Lower baseline cerebral perfusion correlated with poorer baseline efficacy scores. Reduction in cerebral metabolism or whole brain volume correlated with clinical worsening, regardless of treatment assignment.
Tau pathology and cerebral metabolism assessments showed no evidence of lanabecestat slowing pathophysiologic progression of AD. Lanabecestat exposure was associated with brain volume reductions. Correlations between imaging measures and cognitive assessments may aid future study design.
来那贝司他是一种β-分泌酶1(BACE1)抑制剂,曾作为一种潜在的可改变阿尔茨海默病(AD)病情的治疗药物进行研究。如先前报道,淀粉样β蛋白(Aβ)神经炎性斑块负担的减轻并未带来临床益处。本文报告了来那贝司他对神经影像学生物标志物的影响以及神经影像学生物标志物与疗效指标之间的相关性。
AMARANTH和DAYBREAK - ALZ研究分别为期104周和78周,是在早期有症状AD(AMARANTH)和轻度AD痴呆(DAYBREAK - ALZ)患者中开展的多中心、随机、双盲、安慰剂对照的来那贝司他研究。患者被随机(1:1:1)分配,每日接受安慰剂、20mg来那贝司他或50mg来那贝司他(AMARANTH研究,n = 2218;DAYBREAK - ALZ研究,n = 1722)。分别使用氟代贝他吡正电子发射断层扫描(PET)、氟脱氧葡萄糖(FDG)PET、氟 tau 蛋白 PET 和容积磁共振成像(MRI)来测量Aβ神经炎性斑块负担、脑代谢、聚集的 tau 神经原纤维缠结和脑容量。此外,在DAYBREAK - ALZ研究中还进行了氟代贝他吡灌注扫描。疗效指标包括13项阿尔茨海默病评估量表认知子量表、阿尔茨海默病协作研究日常生活活动量表、临床痴呆评定量表总分、功能活动问卷和简易精神状态检查。这些研究因无效而提前终止。
尽管之前观察到来那贝司他可使Aβ神经炎性斑块负担逐年降低,但在聚集的tau神经原纤维缠结负担的年化变化(AMARANTH研究,n = 284;DAYBREAK - ALZ研究,n = 70)、脑代谢(AMARANTH研究,n = 260;DAYBREAK - ALZ研究,n = 38)和灌注(DAYBREAK - ALZ研究,n = 213)方面,各治疗组之间没有差异。与安慰剂相比,来那贝司他治疗组出现了更大程度的脑容量减少(AMARANTH研究,n = 1697 [全脑];DAYBREAK - ALZ研究,n = 650 [全脑])。更高的基线聚集tau神经原纤维缠结负担、更低的脑代谢和更小的脑容量与更差的基线疗效评分以及更大程度的临床恶化相关。更低的基线脑灌注与更差的基线疗效评分相关。脑代谢或全脑容量的减少与临床恶化相关,无论治疗分配如何。
tau病理和脑代谢评估未显示来那贝司他有减缓AD病理生理进展的证据。来那贝司他的暴露与脑容量减少有关。影像学测量与认知评估之间的相关性可能有助于未来的研究设计。
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