Structural highlights
Function
AOFB_HUMAN Catalyzes the oxidative deamination of biogenic and xenobiotic amines and has important functions in the metabolism of neuroactive and vasoactive amines in the central nervous system and peripheral tissues. MAOB preferentially degrades benzylamine and phenylethylamine.
Publication Abstract from PubMed
The major structural difference between human monoamine oxidases A (MAO A) and B (MAO B) is that MAO A has a monopartite substrate cavity of approximately 550 A(3) volume and MAO B contains a dipartite cavity structure with volumes of approximately 290 A(3) (entrance cavity) and approximately 400 A(3) (substrate cavity). Ile199 and Tyr326 side chains separate these two cavities in MAO B. To probe the function of these gating residues, Ile199Ala and Ile199Ala-Tyr326Ala mutant forms of MAO B were investigated. Structural data on the Ile199Ala MAO B mutant show no alterations in active site geometries compared with wild-type enzyme while the Ile199Ala-Tyr326Ala MAO B mutant exhibits alterations in residues 100-103 which are part of the loop gating the entrance to the active site. Both mutant enzymes exhibit catalytic properties with increased amine K(M) but unaltered k(cat) values. The altered K(M) values on mutation are attributed to the influence of the cavity structure in the binding and subsequent deprotonation of the amine substrate. Both mutant enzymes exhibit weaker binding affinities relative to wild-type enzyme for small reversible inhibitors. Ile199Ala MAO B exhibits an increase in binding affinity for reversible MAO B specific inhibitors which bridge both cavities. The Ile199Ala-Tyr326Ala double mutant exhibits inhibitor binding properties more similar to those of MAO A than to MAO B. These results demonstrate that the bipartite cavity structure in MAO B plays an important role in substrate and inhibitor recognition to distinguish its specificities from those of MAO A and provide insights into specific reversible inhibitor design for these membrane-bound enzymes. Database The atomic coordinates and structural factors of the structure of human MAO B Ile199Ala-Tyr326Ala double mutant have been deposited in the Protein Data Bank under the accession number 3zyx.
The 'gating' residues Ile199 and Tyr326 in human monoamine oxidase B function in substrate and inhibitor recognition.,Milczek EM, Binda C, Rovida S, Mattevi A, Edmondson DE FEBS J. 2011 Dec;278(24):4860-9. doi: 10.1111/j.1742-4658.2011.08386.x., Epub 2011 Nov 3. PMID:21978362[1]
From MEDLINE®/PubMed®, a database of the U.S. National Library of Medicine.
See Also
References
- ↑ Milczek EM, Binda C, Rovida S, Mattevi A, Edmondson DE. The 'gating' residues Ile199 and Tyr326 in human monoamine oxidase B function in substrate and inhibitor recognition. FEBS J. 2011 Dec;278(24):4860-9. doi: 10.1111/j.1742-4658.2011.08386.x., Epub 2011 Nov 3. PMID:21978362 doi:10.1111/j.1742-4658.2011.08386.x
