Open AccessFunctionalized Double Strain-Promoted Stapled Peptides for Inhibiting the p53-MDM2 Interaction
Author(s) -
Krishna Sharma,
Alexander V. Strizhak,
Elaine Fowler,
Wenshu Xu,
Ben Chappell,
Hannah F. Sore,
Warren R. J. D. Galloway,
Matthew N. Grayson,
Yu Heng Lau,
Laura S. Itzhaki,
David R. Spring
Publication year - 2020
Publication title -
acs omega
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.779
H-Index - 40
ISSN - 2470-1343
DOI - 10.1021/acsomega.9b03459
Subject(s) - substituent , peptide , reagent , strain (injury) , reactivity (psychology) , stereochemistry , azide , combinatorial chemistry , chemistry , biochemistry , organic chemistry , biology , medicine , alternative medicine , pathology , anatomy
The Sondheimer dialkyne reagent has previously been employed in strain-promoted double-click cycloadditions with bis-azide peptides to generate stapled peptide inhibitors of protein-protein interactions. The substituted variants of the Sondheimer dialkyne can be used to generate functionalized stapled peptide inhibitors with improved biological properties; however, this remains a relatively underdeveloped field. Herein, we report the synthesis of new substituted variants of Sondheimer dialkyne and their application in the stapling of p53-based diazido peptides to generate potent stapled peptide-based inhibitors of the oncogenic p53-MDM2 interaction. The functionalized stapled peptide formed from a meta -fluoro-substituted Sondheimer dialkyne was found to be the most potent inhibitor. Furthermore, through experimental studies and density functional theory calculations, we investigated the impact of the substituent on the strain-promoted double-click reactivity of Sondheimer dialkyne.
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