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Microglia-Based Phenotypic Screening Identifies a Novel Inhibitor of Neuroinflammation Effective in Alzheimer’s Disease Models

Authors :
Xuefei Ji
Guifa Zhong
Lu-Yi Li
Donghai Wu
Xiurong Rao
Kejian Zhang
Dengfeng Xu
Libo Zou
Wenhui Hu
Wei Zhou
Hao Wang
Micky D. Tortorella
Guoqing Sheng
Xing Ji
Sihai Fu
Xiaorong Liu
Shaogao Zeng
Hui Xie
Tianyan Chi
Source :
ACS Chemical Neuroscience. 7:1499-1507
Publication Year :
2016
Publisher :
American Chemical Society (ACS), 2016.

Abstract

Currently, anti-AD drug discovery using target-based approaches is extremely challenging due to unclear etiology of AD and absence of validated therapeutic protein targets. Neuronal death, regardless of causes, plays a key role in AD progression, and it is directly linked to neuroinflammation. Meanwhile, phenotypic screening is making a resurgence in drug discovery process as an alternative to target-focused approaches. Herein, we employed microglia-based phenotypic screenings to search for small molecules that modulate the release of detrimental proinflammatory cytokines. The identified novel pharmacological inhibitor of neuroinflammation (named GIBH-130) was validated to alter phenotypes of neuroinflammation in AD brains. Notably, this molecule exhibited comparable in vivo efficacy of cognitive impairment relief to donepezil and memantine respectively in both β amyloid-induced and APP/PS1 double transgenic Alzheimer's murine models at a substantially lower dose (0.25 mg/kg). Therefore, GIBH-130 constitutes a unique chemical probe for pathogenesis research and drug development of AD, and it also suggests microglia-based phenotypic screenings that target neuroinflammation as an effective and feasible strategy to identify novel anti-AD agents.

Details

ISSN :
19487193
Volume :
7
Database :
OpenAIRE
Journal :
ACS Chemical Neuroscience
Accession number :
edsair.doi.dedup.....fe6bec729a1bbc6f1efc26765e84f06d