An unprecedented reversible mode of action of β-lactams for the inhibition of human fatty acid amide hydrolase (hFAAH)

Marion Feledziak; Catherine Michaux; Didier M Lambert; Jacqueline Marchand-Brynaert

doi:10.1016/j.ejmech.2012.11.035

An unprecedented reversible mode of action of β-lactams for the inhibition of human fatty acid amide hydrolase (hFAAH)

Marion Feledziak, Catherine Michaux, Didier M Lambert, Jacqueline Marchand-Brynaert

Résultats de recherche: Contribution à un journal/une revue › Article › Revue par des pairs

Résumé

A series of compound was prepared to clarify the reversible mechanism of β-lactamic hFAAH inhibitors on the one hand, and to modulate some of their physicochemical parameters on the other hand. In particular, two compounds (4b and 4e) were designed to display a potential good leaving group on the crucial carbonyl with a view to possibly acylating the active serine of the hFAAH catalytic triad. Reversibility studies showed that these two compounds retain the reversible mode of inhibition, suggesting a noncovalent interaction between our β-lactams and hFAAH. Finally, pharmacological evaluations of bioisosteres of the lead compound (4a, IC(50) = 5.3 nM) revealed that log P values and PSA could be optimized without altering the FAAH inhibition (IC(50) values from 3.65 nM to 70.9 nM).

langue originale	Anglais
Pages (de - à)	101-11
Nombre de pages	11
journal	European Journal of Medicinal Chemistry
Volume	60
Les DOIs	https://doi.org/10.1016/j.ejmech.2012.11.035
Etat de la publication	Publié - 2013

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10.1016/j.ejmech.2012.11.035

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@article{ee39edfc83504b38a87046e4afe5263d,

title = "An unprecedented reversible mode of action of β-lactams for the inhibition of human fatty acid amide hydrolase (hFAAH)",

abstract = "A series of compound was prepared to clarify the reversible mechanism of β-lactamic hFAAH inhibitors on the one hand, and to modulate some of their physicochemical parameters on the other hand. In particular, two compounds (4b and 4e) were designed to display a potential good leaving group on the crucial carbonyl with a view to possibly acylating the active serine of the hFAAH catalytic triad. Reversibility studies showed that these two compounds retain the reversible mode of inhibition, suggesting a noncovalent interaction between our β-lactams and hFAAH. Finally, pharmacological evaluations of bioisosteres of the lead compound (4a, IC(50) = 5.3 nM) revealed that log P values and PSA could be optimized without altering the FAAH inhibition (IC(50) values from 3.65 nM to 70.9 nM).",

keywords = "Amidohydrolases, Dose-Response Relationship, Drug, Enzyme Inhibitors, Humans, Models, Molecular, Molecular Structure, Structure-Activity Relationship, beta-Lactams",

author = "Marion Feledziak and Catherine Michaux and Lambert, {Didier M} and Jacqueline Marchand-Brynaert",

year = "2013",

doi = "10.1016/j.ejmech.2012.11.035",

language = "English",

volume = "60",

pages = "101--11",

journal = "European Journal of Medicinal Chemistry",

issn = "0223-5234",

publisher = "Elsevier",

}

TY - JOUR

T1 - An unprecedented reversible mode of action of β-lactams for the inhibition of human fatty acid amide hydrolase (hFAAH)

AU - Feledziak, Marion

AU - Michaux, Catherine

AU - Lambert, Didier M

AU - Marchand-Brynaert, Jacqueline

PY - 2013

Y1 - 2013

N2 - A series of compound was prepared to clarify the reversible mechanism of β-lactamic hFAAH inhibitors on the one hand, and to modulate some of their physicochemical parameters on the other hand. In particular, two compounds (4b and 4e) were designed to display a potential good leaving group on the crucial carbonyl with a view to possibly acylating the active serine of the hFAAH catalytic triad. Reversibility studies showed that these two compounds retain the reversible mode of inhibition, suggesting a noncovalent interaction between our β-lactams and hFAAH. Finally, pharmacological evaluations of bioisosteres of the lead compound (4a, IC(50) = 5.3 nM) revealed that log P values and PSA could be optimized without altering the FAAH inhibition (IC(50) values from 3.65 nM to 70.9 nM).

AB - A series of compound was prepared to clarify the reversible mechanism of β-lactamic hFAAH inhibitors on the one hand, and to modulate some of their physicochemical parameters on the other hand. In particular, two compounds (4b and 4e) were designed to display a potential good leaving group on the crucial carbonyl with a view to possibly acylating the active serine of the hFAAH catalytic triad. Reversibility studies showed that these two compounds retain the reversible mode of inhibition, suggesting a noncovalent interaction between our β-lactams and hFAAH. Finally, pharmacological evaluations of bioisosteres of the lead compound (4a, IC(50) = 5.3 nM) revealed that log P values and PSA could be optimized without altering the FAAH inhibition (IC(50) values from 3.65 nM to 70.9 nM).

KW - Amidohydrolases

KW - Dose-Response Relationship, Drug

KW - Enzyme Inhibitors

KW - Humans

KW - Models, Molecular

KW - Molecular Structure

KW - Structure-Activity Relationship

KW - beta-Lactams

U2 - 10.1016/j.ejmech.2012.11.035

DO - 10.1016/j.ejmech.2012.11.035

M3 - Article

C2 - 23287055

SN - 0223-5234

VL - 60

SP - 101

EP - 111

JO - European Journal of Medicinal Chemistry

JF - European Journal of Medicinal Chemistry

ER -

An unprecedented reversible mode of action of β-lactams for the inhibition of human fatty acid amide hydrolase (hFAAH)

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