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. 2014 Dec 15;15(18):2680-3.
doi: 10.1002/cbic.201402374. Epub 2014 Oct 29.

Linear aliphatic dialkynes as alternative linkers for double-click stapling of p53-derived peptides

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Linear aliphatic dialkynes as alternative linkers for double-click stapling of p53-derived peptides

Yu Heng Lau et al. Chembiochem. .

Abstract

We investigated linear aliphatic dialkynes as a new structural class of i,i+7 linkers for the double-click stapling of p53-based peptides. The optimal combination of azido amino acids and dialkynyl linker length for MDM2 binding was determined. In a direct comparison between aliphatic and aromatic staple scaffolds, the aliphatic staples resulted in superior binding to MDM2 in vitro and superior p53-activating capability in cells when using a diazidopeptide derived from phage display. This work demonstrates that the nature of the staple scaffold is an important factor that can affect peptide bioactivity in cells.

Keywords: anticancer agents; click chemistry; macrocycles; peptides; stapling.

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