• Title of article

    An Integrated Workflow for Proteome-Wide Off-Target Identification and Polypharmacology Drug Design

  • Author/Authors

    Evangelidis, Thomas National and Kapodistrian University of Athens - Faculty of Pharmacy - Department of Pharmaceutical Chemistry, Greece , Xie, Lei City University of New York - Hunter College, The Graduate Center - Department of Computer Science, USA

  • From page
    275
  • To page
    284
  • Abstract
    Polypharmacology, which focuses on designing drugs to target multiple receptors, has emerged as a new paradigm in drug discovery. To rationally design multi-target drugs, it is fundamental to understand protein-ligand interactions on a proteome scale. We have developed a Proteome-wide Off-target Pipeline (POP) that integrates ligand binding site analysis, protein-ligand docking, the statistical analysis of docking scores, and electrostatic potential calculations. The utility of POP is demonstrated by a case study, in which the molecular mechanism of anti-cancer effect of Nelfinavir is hypothesized. By combining structural proteome-wide off-target identification and systems biology, it is possible for us to correlate drug perturbations with clinical outcomes.
  • Keywords
    drug discovery , structural proteomics , polypharmacology , off , target , systems biology
  • Journal title
    Tsinghua Science and Technology
  • Journal title
    Tsinghua Science and Technology
  • Record number

    2535619