Kinetics, mechanism, and inhibition of monoamine oxidase

Rona R Ramsay¹, Alen Albreht^{2

3}

Affiliations

¹ Biomedical Sciences Research Complex, University of St Andrews, North Haugh, St Andrews, KY16 8QP, UK. rrr@st-andrews.ac.uk.
² Department of Food Chemistry, National Institute of Chemistry, Hajdrihova 19, 1000, Ljubljana, Slovenia.
³ Department of Analytical, Environmental and Forensic Sciences, Faculty of Life Sciences and Medicine, King's College London, Franklin-Wilkins Building, London, SE1 8WA, UK.

PMID: 29516165
DOI: 10.1007/s00702-018-1861-9

Review

Kinetics, mechanism, and inhibition of monoamine oxidase

Rona R Ramsay et al. J Neural Transm (Vienna). 2018 Nov.

. 2018 Nov;125(11):1659-1683.

doi: 10.1007/s00702-018-1861-9. Epub 2018 Mar 7.

Authors

Rona R Ramsay¹, Alen Albreht^{2

3}

Affiliations

¹ Biomedical Sciences Research Complex, University of St Andrews, North Haugh, St Andrews, KY16 8QP, UK. rrr@st-andrews.ac.uk.
² Department of Food Chemistry, National Institute of Chemistry, Hajdrihova 19, 1000, Ljubljana, Slovenia.
³ Department of Analytical, Environmental and Forensic Sciences, Faculty of Life Sciences and Medicine, King's College London, Franklin-Wilkins Building, London, SE1 8WA, UK.

PMID: 29516165
DOI: 10.1007/s00702-018-1861-9

Abstract

Monoamine oxidases (MAOs) catalyse the oxidation of neurotransmitter amines and a wide variety of primary, secondary and tertiary amine xenobiotics, including therapeutic drugs. While inhibition of MAO activity in the periphery removes protection from biogenic amines and so is undesirable, inhibition in the brain gives vital antidepressant and behavioural advantages that make MAO a major pharmaceutical target for inhibitor design. In neurodegenerative diseases, MAO inhibitors can help to maintain neurotransmitter levels, making it a common feature in novel multi-target combinations designed to combat Alzheimer's disease, albeit not yet proven clinically. Vital information for inhibitor design comes from an understanding of the structure, mechanism, and kinetics of the catalyst. This review will summarize the kinetic behaviour of MAO A and B and the kinetic evaluation of reversible inhibitors that transiently decrease catalysis. Kinetic parameters and crystal structures have enabled computational approaches to ligand discovery and validation of hits by docking. Kinetics and a wide variety of substrates and inhibitors along with theoretical modelling have also contributed to proposed schemes for the still debated chemical mechanism of amine oxidation. However, most of the marketed MAO drugs are long-lasting irreversible inactivators. The mechanism of irreversible inhibition by hydrazine, cyclopropylamine, and propargylamine drugs will be discussed. The article finishes with some examples of the propargylamine moiety in multi-target ligand design to combat neurodegeneration.

Keywords: Chemical mechanism; Computation and modelling; Enzyme kinetics; Irreversible inhibition; Monoamine neurotransmitters; Multi-target drug design.

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Kinetics, mechanism, and inhibition of monoamine oxidase

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Kinetics, mechanism, and inhibition of monoamine oxidase

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