ID | 115431 |
Author |
Toguchi, Shohei
Kitasato University
Hirose, Tomoyasu
Kitasato University
Fukui, Kiyoshi
Tokushima University
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Sharpless, K. Barry
The Scripps Research Institute
Ōmura, Satoshi
Kitasato University
Sunazuka, Toshiaki
Kitasato University
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Keywords | fragment-based lead discovery
templated reaction
ligand-binding site
drug discovery
triazole formation
ligand affinity
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Content Type |
Journal Article
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Description | In situ click chemistry is a target-guided synthesis approach for discovering novel lead compounds by assembling organic azides and alkynes into triazoles inside the affinity site of target biogenic molecules such as proteins. We report in situ click chemistry screening with human D-amino acid oxidase (hDAO), which led to the identification of a more potent hDAO inhibitor. The hDAO inhibitors have chemotherapeutic potential as antipsychotic agents. The new inhibitor displayed competitive inhibition of hDAO and showed significantly increased inhibitory activity against hDAO compared with that of an anchor molecule of in situ click chemistry.
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Journal Title |
Chemical and Pharmaceutical Bulletin
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ISSN | 00092363
13475223
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NCID | AA00602100
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Publisher | The Pharmaceutical Society of Japan
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Volume | 64
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Issue | 7
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Start Page | 695
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End Page | 703
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Published Date | 2016-07-01
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EDB ID | |
DOI (Published Version) | |
URL ( Publisher's Version ) | |
FullText File | |
language |
eng
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TextVersion |
Publisher
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departments |
Institute of Advanced Medical Sciences
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