• Title of article

    hCB2 Ligand-Interaction Landscape: Cysteine Residues Critical to Biarylpyrazole Antagonist Binding Motif and Receptor Modulation Original Research Article

  • Author/Authors

    Richard W. Mercier، نويسنده , , Xiao-ying Pei، نويسنده , , Lakshmipathi Pandarinathan، نويسنده , , David R. Janero، نويسنده , , Jing Zhang، نويسنده , , Alexandros Makriyannis، نويسنده ,

  • Issue Information
    ماهنامه با شماره پیاپی سال 2010
  • Pages
    11
  • From page
    1132
  • To page
    1142
  • Abstract
    The human cannabinoid 2 GPCR (hCB2) is a prime therapeutic target. To define potential cysteine-related binding motifs critical to hCB2-ligand interaction, a library of hCB2 cysteine-substitution mutants and a novel, high-affinity biarylpyrazole hCB2 antagonist/inverse agonist (AM1336) functionalized to serve as a covalent affinity probe to target cysteine residues within (or in the microenvironment of) its hCB2 binding pocket were generated. The data provide direct experimental demonstration that both hCB2 TMH7 cysteines [i.e., C7.38(284) and C7.42(288)] are critical to optimal hCB2-AM1336 binding interaction and AM1336 pharmacological activity in a cell-based functional assay (cAMP formation). Elongating the AM1336 aliphatic side chain generated another novel hCB2 inverse agonist that binds covalently and selectively to C7.42(288) only. Identification of specific cysteine residues critical to hCB2 ligand interaction and function informs the structure-based design of hCB2-targeted medicines.
  • Journal title
    Chemistry and Biology
  • Serial Year
    2010
  • Journal title
    Chemistry and Biology
  • Record number

    1159943