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Fluorine-18-Labeled Diaryl-azines as Improved β-Amyloid Imaging Tracers: From Bench to First-in-Human Studies.

Yuying LiKaixiang ZhouXiaojun ZhangHailong ZhaoXiaoming WangRuilin DongYan WangBaian ChenXiao-Xin YanJiapei DaiYanying SuiJinming ZhangMeng-Chao Cui
Published in: Journal of medicinal chemistry (2023)
The deposition of β-amyloid (Aβ) in the brain is a pathologic hallmark of Alzheimer's disease (AD), appearing years before the onset of symptoms, and its detection is incorporated into clinical diagnosis. Here, we have discovered and developed a class of diaryl-azine derivatives for detecting Aβ plaques in the AD brain using PET imaging. After a set of comprehensive preclinical assessments, we screened out a promising Aβ-PET tracer, [ 18 F] 92 , with a high binding affinity to the Aβ aggregates, significant binding ability with the AD brain sections, and optimal brain pharmacokinetic properties in rodents and non-human primates. The first-in-human PET study declared that [ 18 F] 92 displayed low white matter uptake and could bind to Aβ pathology for distinguishing AD from healthy control subjects. All these results support that [ 18 F] 92 might become a promising PET tracer for visualizing Aβ pathology in AD patients.
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