iPSC-Based Compound Screening and In Vitro Trials Identify a Synergistic Anti-amyloid β Combination for Alzheimer's Disease

被引:140
作者
Kondo, Takayuki [1 ,2 ]
Imamura, Keiko [1 ,2 ]
Funayama, Misato [1 ]
Tsukita, Kayoko [1 ]
Miyake, Michiyo [1 ,2 ]
Ohta, Akira [1 ]
Woltjen, Knut [1 ,3 ]
Nakagawa, Masato [1 ]
Asada, Takashi [4 ]
Arai, Tetsuaki [4 ]
Kawakatsu, Shinobu [5 ]
Izumi, Yuishin [6 ]
Kaji, Ryuji [6 ]
Iwata, Nobuhisa [7 ,8 ]
Inoue, Haruhisa [1 ,2 ]
机构
[1] Kyoto Univ, Ctr IPS Cell Res & Applicat CiRA, Kyoto 6068507, Japan
[2] RIKEN, BioResource Ctr, Drug Discovery Cellular Basis Dev Team, Kyoto 6068507, Japan
[3] Kyoto Univ, Hakubi Ctr Adv Res, Kyoto 6068501, Japan
[4] Univ Tsukuba, Fac Med, Div Clin Med, Dept Psychiat, Ibaraki 3058575, Japan
[5] Fukushima Med Univ, Aizu Med Ctr, Dept Neuropsychiat, Fukushima 9693492, Japan
[6] Tokushima Univ, Grad Sch, Inst Biomed Sci, Dept Clin Neurosci, Tokushima 7708503, Japan
[7] Nagasaki Univ, Grad Sch Biomed Sci, Dept Genome Based Drug Discovery, Nagasaki 8528521, Japan
[8] Nagasaki Univ, Grad Sch Biomed Sci, Unit Dementia Res & Drug Discovery, Nagasaki 8528521, Japan
关键词
PLURIPOTENT STEM-CELLS; GAMMA-SECRETASE MODULATION; FUNCTIONAL-NEURONS; DIRECT CONVERSION; BACE1; FIBROBLASTS; DIFFERENTIATION; FINGERPRINTS; MEDICINE; LESSONS;
D O I
10.1016/j.celrep.2017.10.109
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
In the process of drug development, in vitro studies do not always adequately predict human-specific drug responsiveness in clinical trials. Here, we applied the advantage of human iPSC-derived neurons, which offer human-specific drug responsiveness, to screen and evaluate therapeutic candidates for Alzheimer's disease (AD). Using AD patient neurons with nearly 100% purity from iPSCs, we established a robust and reproducible assay for amyloid beta peptide (A beta), a pathogenic molecule in AD, and screened a pharmaceutical compound library. We acquired 27 A beta-lowering screen hits, prioritized hits by chemical structure-based clustering, and selected 6 leading compounds. Next, to maximize the anti-A beta effect, we selected a synergistic combination of bromocriptine, cromolyn, and topiramate as an anti-A beta cocktail. Finally, using neurons from familial and sporadic AD patients, we found that the cocktail showed a significant and potent anti-A beta effect on patient cells. This human iPSC-based platform promises to be useful for AD drug development.
引用
收藏
页码:2304 / 2312
页数:9
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