Structural insight into inhibitors of flavin adenine dinucleotide-dependent lysine demethylases

Niwa, Hideaki; Umehara, Takashi

doi:10.1080/15592294.2017.1290032

Cited by 45 publications

(60 citation statements)

References 134 publications

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“…For instance, they inhibit cytochrome P450 enzymes (Hanzlik and Tullman 1982;Khan et al 2013;Salsali et al 2004), copper amine oxidases (Shepard et al 2003), prostacyclin synthase and alcohol dehydrogenase (Talele 2016;Khan et al 2013). More importantly, cyclopropylamines also show cross reactivity with the histone demethylases (Lysine-Specific Demethylase (LSD) 1 and 2) that play a vital role in regulation of gene expression (Schmidt and McCafferty 2007;Binda et al 2010;Niwa and Umehara 2017).…”

Section: Cyclopropylaminesmentioning

confidence: 99%

Kinetics, mechanism, and inhibition of monoamine oxidase

Ramsay

Albreht

2018

J Neural Transm

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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.

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Section: Cyclopropylaminesmentioning

confidence: 99%

Kinetics, mechanism, and inhibition of monoamine oxidase

Ramsay

Albreht

2018

J Neural Transm

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“…11,[13][14][15][16][17] Since LSD1 is involved in tumorigenesis and progression of various cancers, LSD1-specic inhibitors are considered as not only chemical tools for biomedical research, but also as potential anticancer agents. 18,19 Most cell-permeable LSD1 inhibitors reported so far, including ours, 17 are based on the tranylcypromine scaffold, and are irreversible, covalently reacting inhibitors. 15,19 On the other hand, no LSD2-specic inhibitors have yet been developed, which hinders the study of the chemical biology of LSD2.…”

Section: Introductionmentioning

confidence: 97%

Inhibition of FAD-dependent lysine-specific demethylases by chiral polyamine analogues

et al. 2018

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“…To date, a number of LSD1 inhibitors has been developed . LSD1 inhibitors are mainly categorized into two types, irreversible inhibitors and reversible inhibitors.…”

Section: Introductionmentioning

confidence: 99%

“…Thus, the development of LSD1 selective‐inhibitors is highly desired. Currently, several irreversible LSD1 inhibitors [e. g., ORY‐1001 ( 4 ), GSK2879552 ( 5 ), ORY‐2001, INCB‐059872, IMG‐7289 and CC‐90011] are being tested in clinical trials for cancers and neurodegenerative disorders ,…”

Section: Introductionmentioning

confidence: 99%

Drug Design Concepts for LSD1‐Selective Inhibitors

Ota

Suzuki

2018

The Chemical Record

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Lysine‐specific demethylase 1 (LSD1) is one of the flavin‐dependent oxidases and is involved in many cellular processes by controlling the methylation of histone H3. Recently, it has been reported that LSD1 is associated with several diseases such as cancer, metabolic disorders, and psychiatric diseases. Thus, LSD1 is an attractive molecular target for the treatment of these diseases, and its inhibitors are predicted as therapeutic agents. Although a variety of LSD1 inhibitors have been reported to date, many of them show insufficient activities and selectivity toward LSD1. Meanwhile, we identified several LSD1‐selective inhibitors using target‐guided synthesis strategies based on our original ideas. Our LSD1 inhibitors show not only potent LSD1‐selective inhibitory activities, but also unique bioactivities both in vitro and in vivo. This account highlights our drug design concepts for and identification of LSD1‐selective inhibitors.

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Structural insight into inhibitors of flavin adenine dinucleotide-dependent lysine demethylases

Cited by 45 publications

References 134 publications

Kinetics, mechanism, and inhibition of monoamine oxidase

Kinetics, mechanism, and inhibition of monoamine oxidase

Inhibition of FAD-dependent lysine-specific demethylases by chiral polyamine analogues

Drug Design Concepts for LSD1‐Selective Inhibitors

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