Design and exploration of novel boronic acid Inhibitors reveals important Interactions with a clavulanic acid-resistant sulfhydryl- variable (SHV) β‑ lactamase
Articolo
Data di Pubblicazione:
2013
Citazione:
Design and exploration of novel boronic acid Inhibitors reveals important Interactions with a clavulanic acid-resistant sulfhydryl-
variable (SHV) β‑ lactamase / Marisa L., W., Elizabeth A., R., Magdalena A., T., Sarah M., D., Christopher R., B., Krisztina M., P.W., Kerri M., S., Yan, X.u., Jeffrey R., D.S., Romagnoli, C., Caselli, E., Prati, F., Focco Van Den, A., Robert A., B.. - In: JOURNAL OF MEDICINAL CHEMISTRY. - ISSN 0022-2623. - STAMPA. - 56:3(2013), pp. 1084-1097. [10.1021/jm301490d]
Abstract:
Inhibitor resistant (IR) class A β -lactamases pose a signi fi cant threat to
many current antibiotic combinations. The K234R substitution in the SHV β -lactamase,
from Klebsiella pneumoniae, results in resistance to ampicillin/clavulanate. After site-
saturation mutagenesis of Lys-234 in SHV, microbiological and biochemical character-
ization of the resulting β -lactamases revealed that only − Arg conferred resistance to
ampicillin/clavulanate. X-ray crystallography revealed two conformations of Arg-234 and
Ser-130 in SHV K234R. The movement of Ser-130 is the principal cause of the observed
clavulanate resistance. A panel of boronic acid inhibitors was designed and tested against
SHV-1 and SHV K234R. A chiral ampicillin analogue was discovered to have a 2.4 ± 0.2
nM K i for SHV K234R; the chiral ampicillin analogue formed a more complex hydrogen-
bonding network in SHV K234R vs SHV-1. Consideration of the spatial position of Ser-
130 and Lys-234 and this hydrogen-bonding network will be important in the design of
novel antibiotics targeting IR β -lactamases.
many current antibiotic combinations. The K234R substitution in the SHV β -lactamase,
from Klebsiella pneumoniae, results in resistance to ampicillin/clavulanate. After site-
saturation mutagenesis of Lys-234 in SHV, microbiological and biochemical character-
ization of the resulting β -lactamases revealed that only − Arg conferred resistance to
ampicillin/clavulanate. X-ray crystallography revealed two conformations of Arg-234 and
Ser-130 in SHV K234R. The movement of Ser-130 is the principal cause of the observed
clavulanate resistance. A panel of boronic acid inhibitors was designed and tested against
SHV-1 and SHV K234R. A chiral ampicillin analogue was discovered to have a 2.4 ± 0.2
nM K i for SHV K234R; the chiral ampicillin analogue formed a more complex hydrogen-
bonding network in SHV K234R vs SHV-1. Consideration of the spatial position of Ser-
130 and Lys-234 and this hydrogen-bonding network will be important in the design of
novel antibiotics targeting IR β -lactamases.
Tipologia CRIS:
Articolo su rivista
Keywords:
BETA-LACTAMASE; boronic acids; enzyme inhibitor; X-RAY DIFFRACTION STRUCTURE
Elenco autori:
Marisa L., Winkler; Elizabeth A., Rodkey; Magdalena A., Taracila; Sarah M., Drawz; Christopher R., Bethel; Krisztina M., Papp Wallace; Kerri M., Smith; Yan, Xu; Jeffrey R., Dwulit Smith; Romagnoli, Chiara; Caselli, Emilia; Prati, Fabio; Focco Van Den, Akker; Robert A., Bonomo
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