Crystal Structures of KPC-2 and SHV-1 β-Lactamases in Complex with the Boronic Acid Transition State Analog S02030

Nguyen, Nhu; Krishnan, Nikhil; Rojas, Laura; Prati, Fabio; Caselli, Emilia; Romagnoli, Chiara; Akker, F. van den

doi:10.1128/aac.02643-15

Cited by 33 publications

(39 citation statements)

References 34 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Overall, both derivatives 2 and 4 adopt a deacylation transition‐state analogue conformation with an inverted boron configuration. In such a conformation, previously described for other class A BLs, the positions of the boronic acid oxygen atoms are as follows: one is located in the oxyanion hole and the other one displaces the deacylation water normally positioned between Glu‐166 and Asn‐170 …”

Section: Resultsmentioning

confidence: 95%

“…In a possible derivatization of phenylboronic acid ( 1 ), we reasoned that the introduction of a carboxylic group mimicking the C3(4)′ carboxylate of β‐lactam antibiotics, a key recognition feature in BLs, might improve KCP‐2 binding through a large interaction network with Arg‐220, Ser‐130, Thr‐237, and Thr‐235. All mentioned residues are located in the β‐lactam carboxylate binding pocket, in which the sulfate group of avibactam, as well as the carboxylic group of other known class A inhibitors, are known to bind …”

Section: Resultsmentioning

confidence: 99%

“…All mentioned residues are located in the b-lactam carboxylate binding pocket, in which the sulfate group of avibactam, as well as the carboxylic group of otherk nownc lass Ai nhibitors, are knowntob ind. [17,27] Whereast he presence of the boronic acid group guarantees covalentl inking to Ser-70, sinking de facto the inhibitor in the active site, ap roperl inker could correctly orient the lateralc arboxylic chain in the targeted site without preventing other classical interactions between the ligand and the Thr-237, Glu-166, and Asn-170 residues,a ss een in the KPC-2-3-nitrophenylboronic acid complex. [26] With the purpose of mimicking distance, chemistry,a nd interactions of the C3(4)' carboxylate of b-lactam antibiotics, structuralc onsiderations suggested to introduce ac arboxylic moiety,p roperly spaced by at wo atomic vinyl chain,i nt he ortho positiona djacent to the boronic group of compound 1.…”

Section: Design and Synthesismentioning

confidence: 99%

“…In such ac onformation, previously described for other class AB Ls, the positions of the boronic acid oxygen atoms are as follows:o ne is located in the oxyanion hole and the other one displaces the deacylation water normally positioned between Glu-166 and Asn-170. [27,34] Compound 2 orients its phenylr ing against one hydrophobic region defined by Trp-105 andL eu-167 in proximity of the opening of the binding site. The phenylr ing of 2 is involved in cation-p and p-p interactions with Asn-132 and Trp-105, respectively.F inally,a se xpected, 2 orientsi ts ortho carboxyvinyl lateral chain toward the C3(4')c arboxylate binding pocket, highly conserved in all serine BLs.…”

Section: Crystal Structures Of the Kpc-2-2 And Kpc-2-4 Complexesmentioning

confidence: 99%

See 3 more Smart Citations

Phenylboronic Acid Derivatives as Validated Leads Active in Clinical Strains Overexpressing KPC‐2: A Step against Bacterial Resistance

et al. 2018

View full text Add to dashboard Cite

The emergence and dissemination of multidrug resistant (MDR) pathogens resistant to nearly all available antibiotics poses a significant threat in clinical therapy. Among them, Klebsiella pneumoniae clinical isolates overexpressing KPC-2 carbapenemase are the most worrisome, extending bacterial resistance to last-resort carbapenems. In this study, we investigate the molecular recognition requirements in the KPC-2 active site by small phenylboronic acid derivatives. Four new phenylboronic acid derivatives were designed and tested against KPC-2. For the most active, despite their simple chemical structures, nanomolar affinity was achieved. The new derivatives restored susceptibility to meropenem in clinical strains overexpressing KPC-2. Moreover, no cytotoxicity was detected in cell-viability assays, which further validated the designed leads. Two crystallographic binary complexes of the best inhibitors binding KPC-2 were obtained at high resolution. Kinetic descriptions of slow binding, time-dependent inhibition, and interaction geometries in KPC-2 were fully investigated. This study will ultimately lead toward the optimization and development of more-effective KPC-2 inhibitors.

show abstract

Section: Resultsmentioning

confidence: 95%

Section: Resultsmentioning

confidence: 99%

Section: Design and Synthesismentioning

confidence: 99%

Section: Crystal Structures Of the Kpc-2-2 And Kpc-2-4 Complexesmentioning

confidence: 99%

See 2 more Smart Citations

Phenylboronic Acid Derivatives as Validated Leads Active in Clinical Strains Overexpressing KPC‐2: A Step against Bacterial Resistance

et al. 2018

View full text Add to dashboard Cite

show abstract

“…In the study described in the companion article, the crystal structure of KPC-2 and SHV-1 with 2b (S02030) revealed multiple conformations of 2b in the active site of KPC-2 and SHV-1 (25). The boronic acid preserved the tetrahedral interactions, forming the bond with catalytic serine, positioning one of the boronic acid oxygens in the oxyanion hole (T237:N for KPC-2) and the other toward S130.…”

Section: Resultsmentioning

confidence: 99%

Boronic Acid Transition State Inhibitors Active against KPC and Other Class A β-Lactamases: Structure-Activity Relationships as a Guide to Inhibitor Design

Rojas

Taracila

Papp-Wallace

et al. 2016

Antimicrob Agents Chemother

Self Cite

View full text Add to dashboard Cite

g Boronic acid transition state inhibitors (BATSIs) are competitive, reversible ␤-lactamase inhibitors (BLIs). In this study, a series of BATSIs with selectively modified regions (R1, R2, and amide group) were strategically designed and tested against representative class A ␤-lactamases of Klebsiella pneumoniae, KPC-2 and SHV-1. Firstly, the R1 group of compounds 1a to 1c and 2a to 2e mimicked the side chain of cephalothin, whereas for compounds 3a to 3c, 4a, and 4b, the thiophene ring was replaced by a phenyl, typical of benzylpenicillin. Secondly, variations in the R2 groups which included substituted aryl side chains (compounds 1a, 1b, 1c, 3a, 3b, and 3c) and triazole groups (compounds 2a to 2e) were chosen to mimic the thiazolidine and dihydrothiazine ring of penicillins and cephalosporins, respectively. Thirdly, the amide backbone of the BATSI, which corresponds to the amide at C-6 or C-7 of ␤-lactams, was also changed to the following bioisosteric groups: urea (compound 3b), thiourea (compound 3c), and sulfonamide (compounds 4a and 4b). Among the compounds that inhibited KPC-2 and SHV-1 ␤-lactamases, nine possessed 50% inhibitory concentrations (IC 50 s) of <600 nM. The most active compounds contained the thiopheneacetyl group at R1 and for the chiral BATSIs, a carboxy-or hydroxy-substituted aryl group at R2. The most active sulfonamido derivative, compound 4b, lacked an R2 group. Compound 2b (S02030) was the most active, with acylation rates (k 2 /K) of 1.2 ؎ 0.2 ؋ 10 4 M ؊1 s ؊1 for KPC-2 and 4.7 ؎ 0.6 ؋ 10 3 M ؊1 s ؊1 for SHV-1, and demonstrated antimicrobial activity against Escherichia coli DH10B carrying bla SHV variants and bla KPC-2 or bla KPC-3 and against clinical strains of Klebsiella pneumoniae and E. coli producing different class A ␤-lactamase genes. At most, MICs decreased from 16 to 0.5 mg/liter.

show abstract

Thiophene‐containing compounds with antimicrobial activity

Roman¹

2022

Archiv der Pharmazie

View full text Add to dashboard Cite

Thiophene, as a member of the group of five-membered heterocycles containing one heteroatom, is one of the simplest heterocyclic systems. Many synthetic strategies allow the accurate positioning of various functionalities onto the thiophene ring. This review provides a comprehensive, systematic and detailed account of the developments in the field of antimicrobial compounds featuring at least one thiophene ring in their structure, over the last decade.

show abstract

Crystal Structures of KPC-2 and SHV-1 β-Lactamases in Complex with the Boronic Acid Transition State Analog S02030

Cited by 33 publications

References 34 publications

Phenylboronic Acid Derivatives as Validated Leads Active in Clinical Strains Overexpressing KPC‐2: A Step against Bacterial Resistance

Phenylboronic Acid Derivatives as Validated Leads Active in Clinical Strains Overexpressing KPC‐2: A Step against Bacterial Resistance

Boronic Acid Transition State Inhibitors Active against KPC and Other Class A β-Lactamases: Structure-Activity Relationships as a Guide to Inhibitor Design

Thiophene‐containing compounds with antimicrobial activity

Contact Info

Product

Resources

About