Metallo-β-lactamase inhibitors by bioisosteric replacement: preparation, activity and binding
Permanent link
https://hdl.handle.net/10037/12626DOI
dx.doi.org/10.1016/j.ejmech.2017.04.035Date
2017-04-14Type
Journal articleTidsskriftartikkel
Peer reviewed
Author
Skagseth, Susann; Akhter, Sundus; Paulsen, Marianne H; Muhammad, Zeeshan; Samuelsen, Ørjan; Leiros, Hanna-Kirsti S.; Bayer, AnnetteAbstract
Bacterial resistance is compromising the use of β-lactam antibiotics including carbapenems. The
main resistance mechanism against β-lactams is hydrolysis of the β-lactam ring mediated by
serine- or metallo-β-lactamases (MBLs). Although several inhibitors of MBLs have been
reported, none has been developed into a clinically useful inhibitor. Mercaptocarboxylic acids
are among the most prominent scaffolds reported as MBL inhibitors. In this study, the
carboxylate group of mercaptocarboxylic acids was replaced with bioisosteric groups like
phosphonate esters, phosphonic acids and NH-tetrazoles. The influence of the replacement on
the bioactivity and inhibitor binding was evaluated. A series of bioisosteres of previously
reported inhibitors was synthesized and evaluated against the MBLs VIM-2, NDM-1 and GIM-
1. The most active inhibitors combined a mercapto group and a phosphonate ester or acid, with
two/three carbon chains connecting a phenyl group. Surprisingly, also compounds containing
thioacetate groups instead of thiols showed low IC50 values. High-resolution crystal structures of
three inhibitors in complex with VIM-2 revealed hydrophobic interactions for the diethyl groups
in the phosphonate ester (inhibitor 2b), the mercapto bridging the two active site zinc ions, and
tight stacking of the benzene ring to the inhibitor between Phe62, Tyr67, Arg228 and His263.
The inhibitors show reduced enzyme activity in Escherichia coli cells harboring MBL. The
obtained results will be useful for further structural guided design of MBL inhibitors.
Description
Accepted manuscript version, licensed CC BY-NC-ND 4.0. " . Published version available in European Journal of Medicinal Chemistry. 135:159-173.
Publisher
ElsevierCitation
Skagseth, S., Akhter, S., Paulsen, M. H., Muhammad, Z., Samuelsen, Ø., Leiros, H. & Bayer, A. (2017). Metallo-β-lactamase inhibitors by bioisosteric replacement: preparation, activity and binding. European Journal of Medicinal Chemistry. 135:159-173. https://doi.org/10.1016/j.ejmech.2017.04.035Metadata
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