A Cyclized Helix-Loop-Helix Peptide as a Molecular Scaffold for the Design of Inhibitors of Intracellular Protein-Protein Interactions by Epitope and Arginine Grafting
  • Fujiwara, Daisuke
  • Kitada, Hidekazu
  • Oguri, Masahiro
  • Nishihara, Toshio
  • Michigami, Masataka
  • 외 10명
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초록

The design of inhibitors of intracellular protein-protein interactions (PPIs) remains a challenge in chemical biology and drug discovery. We propose a cyclized helix-loop-helix (cHLH) peptide as a scaffold for generating cell-permeable PPI inhibitors through bifunctional grafting: epitope grafting to provide binding activity, and arginine grafting to endow cell-permeability. To inhibit p53-HDM2 interactions, the p53 epitope was grafted onto the C-terminal helix and six Arg residues were grafted onto another helix. The designed peptide cHLHp53-R showed high inhibitory activity for this interaction, and computational analysis suggested a binding mode for HDM2. Confocal microscopy of cells treated with fluorescently labeled cHLHp53-R revealed cell membrane penetration and cytosolic localization. The peptide inhibited the growth of HCT116 and LnCap cancer cells. This strategy of bifunctional grafting onto a well-structured peptide scaffold could facilitate the generation of inhibitors for intracellular PPIs.

키워드

cell-penetrating peptidesepitope graftinghelix-loop-helix peptidesinhibitorsprotein-protein interactionsTUMOR-SUPPRESSOR PATHWAYIN-VIVO ACTIVATIONP53-MDM2 INTERACTIONCANCER-THERAPYP53MDM2ANTAGONISTSSELECTIONLIBRARYDOMAIN
제목
A Cyclized Helix-Loop-Helix Peptide as a Molecular Scaffold for the Design of Inhibitors of Intracellular Protein-Protein Interactions by Epitope and Arginine Grafting
저자
Fujiwara, DaisukeKitada, HidekazuOguri, MasahiroNishihara, ToshioMichigami, MasatakaShiraishi, KazunoriYuba, EijiNakase, IkuhikoIm, HaeriCho, SunheeJoung, Jong YoungKodama, SeijiKono, KenjiHam, SihyunFujii, Ikuo
DOI
10.1002/anie.201603230
발행일
2016-08
유형
Article
저널명
Angewandte Chemie - International Edition
55
36
페이지
10612 ~ 10615