A one-two punch targeting reactive oxygen species and fibril for rescuing Alzheimer’s disease

Author:

Wang Jiefei,Shangguan Ping,Chen Xiaoyu,Zhong YongORCID,Lin Ming,He Mu,Liu Yisheng,Zhou Yuan,Pang Xiaobin,Han Lulu,Lu Mengya,Wang Xiao,Liu YangORCID,Yang Huiqing,Chen Jingyun,Song Chenhui,Zhang JingORCID,Wang XinORCID,Shi BingyangORCID,Tang Ben ZhongORCID

Abstract

AbstractToxic amyloid-beta (Aβ) plaque and harmful inflammation are two leading symptoms of Alzheimer’s disease (AD). However, precise AD therapy is unrealizable due to the lack of dual-targeting therapy function, poor BBB penetration, and low imaging sensitivity. Here, we design a near-infrared-II aggregation-induced emission (AIE) nanotheranostic for precise AD therapy. The anti-quenching emission at 1350 nm accurately monitors the in vivo BBB penetration and specifically binding of nanotheranostic with plaques. Triggered by reactive oxygen species (ROS), two encapsulated therapeutic-type AIE molecules are controllably released to activate a self-enhanced therapy program. One specifically inhibits the Aβ fibrils formation, degrades Aβ fibrils, and prevents the reaggregation via multi-competitive interactions that are verified by computational analysis, which further alleviates the inflammation. Another effectively scavenges ROS and inflammation to remodel the cerebral redox balance and enhances the therapy effect, together reversing the neurotoxicity and achieving effective behavioral and cognitive improvements in the female AD mice model.

Funder

National Natural Science Foundation of China

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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