Stereoisomerism of stapled peptide inhibitors of the p53-Mdm2 interaction: an assessment of synthetic strategies and activity profiles.
Tsz Ying YuenChristopher J BrownYuezhen XueYaw Sing TanFernando J Ferrer GagoXue Er LeeJin Yong NeoDawn TheanHung Yi Kristal KaanAnthony W PartridgeChandra Shekhar VermaDavid Philip LaneCharles W JohannesPublished in: Chemical science (2019)
All-hydrocarbon, i, i+7 stapled peptide inhibitors of the p53-Mdm2 interaction have emerged as promising new leads for cancer therapy. Typical chemical synthesis via olefin metathesis results in the formation of both E- and Z-isomers, an observation that is rarely disclosed but may be of importance in targeting PPI. In this study, we evaluated the effect of staple geometry on the biological activity of five p53-reactivating peptides. We also present strategies for the modulation of the E/Z ratio and attainment of the hydrogenated adduct through repurposing of the metathesis catalyst.