Macrocyclic peptide-based inhibition and imaging of hepatocyte growth factor.
Katsuya SakaiToby PassiouraHiroki SatoKenichiro ItoHiroki FuruhashiMasataka UmitsuJunichi TakagiYukinari KatoHidefumi MukaiShota WarashinaMaki ZoudaYasuyoshi WatanabeSeiji YanoMikihiro ShibataHiroaki SugaKunio MatsumotoPublished in: Nature chemical biology (2019)
Activation of hepatocyte growth factor (HGF) by proteolytic processing is triggered in cancer microenvironments, and subsequent signaling through the MET receptor is involved in cancer progression. However, the structure of HGF remains elusive, and few small/medium-sized molecules can modulate HGF. Here, we identified HiP-8, a macrocyclic peptide consisting of 12 amino acids, which selectively recognizes active HGF. Biochemical analysis and real-time single-molecule imaging by high-speed atomic force microscopy demonstrated that HiP-8 restricted the dynamic domains of HGF into static closed conformations, resulting in allosteric inhibition. Positron emission tomography using HiP-8 as a radiotracer enabled noninvasive visualization and simultaneous inhibition of HGF-MET activation status in tumors in a mouse model. Our results illustrate the conformational change in proteolytic activation of HGF and its detection and inhibition by a macrocyclic peptide, which may be useful for diagnosis and treatment of cancers.
Keyphrases
- growth factor
- atomic force microscopy
- single molecule
- high speed
- positron emission tomography
- high resolution
- computed tomography
- mouse model
- papillary thyroid
- total hip arthroplasty
- amino acid
- pet imaging
- small molecule
- tyrosine kinase
- liver injury
- molecular dynamics simulations
- young adults
- fluorescence imaging
- sensitive detection
- drug induced
- real time pcr