• Title of article

    Biotinyl-methyl 4-(amidomethyl)benzoate is a competitive inhibitor of human biotinidase

  • Author/Authors

    Keyna A. Kobza، نويسنده , , Kittichai Chaiseeda، نويسنده , , Gautam Sarath، نويسنده , , James M. Takacs، نويسنده , , Janos Zempleni، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2008
  • Pages
    7
  • From page
    826
  • To page
    832
  • Abstract
    Posttranslational modification of histones by biotinylation can be catalyzed by both biotinidase (BTD) and holocarboxylase synthetase. Biotinylation of histones is an important epigenetic mechanism to regulate gene expression, DNA repair, and chromatin remodeling. The role of BTD in histone biotinylation is somewhat ambiguous, given that BTD also catalyzes removal of the biotin tag from histones. Here, we sought to develop BTD inhibitors for future studies of the role of BTD in altering chromatin structure. We adopted an existing colorimetric BTD assay for use in a novel 96-well plate format to permit high-throughput screening of potential inhibitors. Biotin analogs were chemically synthesized and tested for their ability to inhibit human BTD. Seven of these compounds inhibited BTD by 26–80%. Biotinyl-methyl 4-(amidomethyl)benzoate had the largest effect on BTD, causing an 80% inhibition at 1 mM concentration. Enzyme kinetics studies were conducted to determine Vmax, Km and Ki for the seven inhibitors; kinetics were consistent with the hypothesis that biotinyl-methyl 4-(amidomethyl)benzoate and the other compounds acted by competitive inhibition of BTD. Finally, biotinyl-methyl 4-(amidomethyl)benzoate did not affect biotin transport in human cells, suggesting specificity in regard to biotin-related processes.
  • Keywords
    Biotinidase , Biotinyl-methyl 4-amidomethyl benzoate , Inhibitors , Histones
  • Journal title
    The Journal of Nutritional Biochemistry
  • Serial Year
    2008
  • Journal title
    The Journal of Nutritional Biochemistry
  • Record number

    1299462