Schließen
  • search hit 1 of 13
Back to Result List

Structural insights into xenobiotic and inhibitor binding to human aldehyde oxidase

  • Aldehyde oxidase (AOX) is a xanthine oxidase (XO)-related enzyme with emerging importance due to its role in the metabolism of drugs and xenobiotics. We report the first crystal structures of human AOX1, substrate free (2.6-angstrom resolution) and in complex with the substrate phthalazine and the inhibitor thioridazine (2.7-angstrom resolution). Analysis of the protein active site combined with steady-state kinetic studies highlight the unique features, including binding and substrate orientation at the active site, that characterize human AOX1 as an important drug-metabolizing enzyme. Structural analysis of the complex with the noncompetitive inhibitor thioridazine revealed a new, unexpected and fully occupied inhibitor-binding site that is structurally conserved among mammalian AOXs and XO. The new structural insights into the catalytic and inhibition mechanisms of human AOX that we now report will be of great value for the rational analysis of clinical drug interactions involving inhibition of AOX1 and for the prediction andAldehyde oxidase (AOX) is a xanthine oxidase (XO)-related enzyme with emerging importance due to its role in the metabolism of drugs and xenobiotics. We report the first crystal structures of human AOX1, substrate free (2.6-angstrom resolution) and in complex with the substrate phthalazine and the inhibitor thioridazine (2.7-angstrom resolution). Analysis of the protein active site combined with steady-state kinetic studies highlight the unique features, including binding and substrate orientation at the active site, that characterize human AOX1 as an important drug-metabolizing enzyme. Structural analysis of the complex with the noncompetitive inhibitor thioridazine revealed a new, unexpected and fully occupied inhibitor-binding site that is structurally conserved among mammalian AOXs and XO. The new structural insights into the catalytic and inhibition mechanisms of human AOX that we now report will be of great value for the rational analysis of clinical drug interactions involving inhibition of AOX1 and for the prediction and design of AOX-stable putative drugs.show moreshow less

Export metadata

Additional Services

Search Google Scholar Statistics
Metadaten
Author details:Catarina Coelho, Alessandro Foti, Tobias Hartmann, Teresa Santos-Silva, Silke LeimkühlerORCiDGND, Maria Joao Romao
DOI:https://doi.org/10.1038/NCHEMBIO.1895
ISSN:1552-4450
ISSN:1552-4469
Pubmed ID:https://pubmed.ncbi.nlm.nih.gov/26322824
Title of parent work (English):Nature chemical biology
Publisher:Nature Publ. Group
Place of publishing:New York
Publication type:Article
Language:English
Year of first publication:2015
Publication year:2015
Release date:2017/03/27
Volume:11
Issue:10
Number of pages:7
First page:779
Last Page:+
Funding institution:Fundacao para a Ciencia e Tecnologia (FCT-MEC) [UID/Multi/04378/2013, EXCL/QEQ-COM/0394/2012, PTDC/BIA-PRO/118377/2010, SFRH/BPD/84581/2012, DAAD-441.00]; Deutsche Forschungsgemeinschaft Grant [Le1171/8-1]; European Community [283570]
Organizational units:Mathematisch-Naturwissenschaftliche Fakultät / Institut für Biochemie und Biologie
Peer review:Referiert

KOBV Logo  OAI Logo  DINI Zertifikat 2007  OA Netzwerk Logo

Accept ✔
This website uses technically necessary session cookies. By continuing to use the website, you agree to this. You can find our privacy policy here.