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Harnessing the PD-L1 interface peptide for positron emission tomography imaging of the PD-1 immune checkpoint.

Kuan HuLin XieMasayuki HanyuYiding ZhangLingyun LiXiaohui MaKotaro NagatsuHisashi SuzukiWeizhi WangMing-Rong Zhang
Published in: RSC chemical biology (2020)
Interface peptides that mediate protein-protein interactions (PPI) are a class of important lead compounds for designing PPI inhibitors. However, their potential as precursors for radiotracers has never been exploited. Here we report that the interface peptides from programmed death-ligand 1 (PD-L1) can be used in positron emission tomography (PET) imaging of programmed cell death 1 (PD-1) with high accuracy and sensitivity. Moreover, the performance differentiation between murine PD-L1 derived interface peptide (mPep-1) and human PD-L1 derived interface peptide (hPep-1) as PET tracers for PD-1 unveiled an unprecedented role of a non-critical residue in target binding, highlighting the significance of PET imaging as a companion diagnostic in drug development. Collectively, this study not only provided a first-of-its-kind peptide-based PET tracer for PD-1 but also conveyed a unique paradigm for developing imaging agents for highly challenging protein targets, which could be used to identify other protein biomarkers involved in the PPI networks.
Keyphrases
  • pet imaging
  • positron emission tomography
  • computed tomography
  • protein protein
  • pet ct
  • amino acid
  • high resolution
  • small molecule
  • binding protein
  • machine learning
  • risk assessment
  • human health
  • dna binding