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Negative Cooperativity in NAD(P)H Quinone Oxidoreductase 1 (NQO1).

Clare F MegarityHoda Abdel-Aal BettleyM Clare CaraherKatherine A ScottRoger C WhiteheadThomas A JowittAldo GutierrezRichard A BryceKaren A NolanIan J StratfordDavid J Timson
Published in: Chembiochem : a European journal of chemical biology (2019)
NAD(P)H quinone oxidoreductase-1 (NQO1) is a homodimeric protein that acts as a detoxifying enzyme or as a chaperone protein. Dicourmarol interacts with NQO1 at the NAD(P)H binding site and can both inhibit enzyme activity and modulate the interaction of NQO1 with other proteins. We show that the binding of dicoumarol and related compounds to NQO1 generates negative cooperativity between the monomers. This does not occur in the presence of the reducing cofactor, NAD(P)H, alone. Alteration of Gly150 (but not Gly149 or Gly174) abolished the dicoumarol-induced negative cooperativity. Analysis of the dynamics of NQO1 with the Gaussian network model indicates a high degree of collective motion by monomers and domains within NQO1. Ligand binding is predicted to alter NQO1 dynamics both proximal to the ligand binding site and remotely, close to the second binding site. Thus, drug-induced modulation of protein motion might contribute to the biological effects of putative inhibitors of NQO1.
Keyphrases
  • drug induced
  • liver injury
  • binding protein
  • protein protein
  • high glucose
  • mass spectrometry
  • endothelial cells
  • heat shock protein
  • transcription factor
  • high resolution
  • heat shock
  • adverse drug
  • endoplasmic reticulum