iPSC-Based Compound Screening and In Vitro Trials Identify a Synergistic Anti-amyloid β Combination for Alzheimer’s Disease
Author(s) -
Takayuki Kondo,
Keiko Imamura,
Misato Funayama,
Kayoko Tsukita,
Michiyo Miyake,
Akira Ohta,
Knut Woltjen,
Masato Nakagawa,
Takashi Asada,
Tetsuaki Arai,
Shinobu Kawakatsu,
Yuishin Izumi,
Ryuji Kaji,
Nobuhisa Iwata,
Haruhisa Inoue
Publication year - 2017
Publication title -
cell reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 6.264
H-Index - 154
eISSN - 2639-1856
pISSN - 2211-1247
DOI - 10.1016/j.celrep.2017.10.109
Subject(s) - drug discovery , induced pluripotent stem cell , drug , pharmacology , drug development , in vitro , amyloid precursor protein , disease , clinical trial , medicine , amyloid (mycology) , alzheimer's disease , computational biology , biology , bioinformatics , biochemistry , pathology , gene , embryonic stem cell
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 β peptide (Aβ), a pathogenic molecule in AD, and screened a pharmaceutical compound library. We acquired 27 Aβ-lowering screen hits, prioritized hits by chemical structure-based clustering, and selected 6 leading compounds. Next, to maximize the anti-Aβ effect, we selected a synergistic combination of bromocriptine, cromolyn, and topiramate as an anti-Aβ cocktail. Finally, using neurons from familial and sporadic AD patients, we found that the cocktail showed a significant and potent anti-Aβ effect on patient cells. This human iPSC-based platform promises to be useful for AD drug development.
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