• Title of article

    Probing reactivity and substrate specificity of both subunits of the dimeric Mycobacterium tuberculosis FabH using alkyl-CoA disulfide inhibitors and acyl-CoA substrates

  • Author/Authors

    Sachdeva، نويسنده , , Sarbjot and Musayev، نويسنده , , Faik and Alhamadsheh، نويسنده , , Mamoun M. and Neel Scarsdale، نويسنده , , J. and Tonie Wright، نويسنده , , H. Glenn Reynolds، نويسنده , , Kevin A.، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2008
  • Pages
    6
  • From page
    85
  • To page
    90
  • Abstract
    The dimeric Mycobacterium tuberculosis FabH (mtFabH) catalyses a Claisen-type condensation between an acyl-CoA and malonyl-acyl carrier protein (ACP) to initiate the Type II fatty acid synthase cycle. To analyze the initial covalent acylation of mtFabH with acyl-CoA, we challenged it with mixture of C6-C20 acyl-CoAs and the ESI-MS analysis showed reaction at both subunits and a strict specificity for C12 acyl CoA. Crystallographic and ESI-MS studies of mtFabH with a decyl-CoA disulfide inhibitor revealed a decyl chain bound in acyl-binding channels of both subunits through disulfide linkage to the active site cysteine. These data provide the first unequivocal evidence that both subunits of mtFabH can react with substrates or inhibitor. The discrepancy between the observed C12 acyl-CoA substrate specificity in the initial acylation step and the higher catalytic efficiency of mtFabH for C18-C20 acyl-CoA substrates in the overall mtFabH catalyzed reaction suggests a role for M. tuberculosis ACP as a specificity determinant in this reaction.
  • Keywords
    Mycobacterium tuberculosis , Mycolic acids , FabH , crystal structure , Fatty acid biosynthesis , Alkyl-CoA disulfide , mass spectrometry
  • Journal title
    Bioorganic Chemistry: an International Journal
  • Serial Year
    2008
  • Journal title
    Bioorganic Chemistry: an International Journal
  • Record number

    1385987