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Design, Synthesis, and Biological Evaluation of Imidazopyrazinone Derivatives as Antagonists of Inhibitor of Apoptosis Proteins (IAPs)

Authors
Kim, J[Kim, Jisook]Bae, I[Bae, Inhwan]Song, J[Song, Jiyoung]Kim, Y[Kim, Younghoon]Ahn, Y[Ahn, Younggil]Park, HJ[Park, Hyun-Ju]Kim, HH[Kim, Ha Hyung]Kim, DK[Kim, Dae Kyong]
Issue Date
Jun-2021
Publisher
WILEY-V C H VERLAG GMBH
Keywords
Imidazopyrazinone; Inhibitors of apoptosis proteins antagonist; Second mitochondrial activator of caspases; Apoptosis
Citation
BULLETIN OF THE KOREAN CHEMICAL SOCIETY, v.42, no.6, pp.847 - 851
Indexed
SCIE
SCOPUS
KCI
Journal Title
BULLETIN OF THE KOREAN CHEMICAL SOCIETY
Volume
42
Number
6
Start Page
847
End Page
851
URI
https://scholarworks.bwise.kr/skku/handle/2021.sw.skku/1977
DOI
10.1002/bkcs.12271
ISSN
0253-2964
Abstract
Apoptosis inhibitor (IAP) proteins are overexpressed in many cancers and implicated in tumor growth, so the development of antagonist that disrupts with the binding of IAP to their partner protein is a promising therapeutic strategy. In an effort to increase cellular activity and improve favorable drug-like properties, we newly designed and synthesized monovalent analogues based on imidazopyrazinone structure of 9. Optimization of cellular potency led to the identification of 17, which showed increase of submicromolar activity (GI(50) = 234 nM) and caspase-3 activation (6.3-fold) in MDA-MB-231 breast cancer cells. These findings clearly show the potential for 17 as a promising monovalent antagonist for the development of an effective anticancer treatment.
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