2008
DOI: 10.1021/ja8029448
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Co-opting the Cell Wall in Fighting Methicillin-Resistant Staphylococcus aureus: Potent Inhibition of PBP 2a by Two Anti-MRSA β-Lactam Antibiotics

Abstract: The second generation of penicillins (including methicillin) was introduced to the clinic in 1959, and by 1961 strains of methicillin-resistant Staphylococcus aureus (MRSA) had emerged. 1 β-Lactam antibiotics were the standard treatment for staphylococcal infections prior to the emergence of MRSA. MRSA is now a global health threat, 2 and community-acquired MRSA has become a significant challenge in the clinic. 2 β-Lactams, which include penicillins, cephalosporins, and carbapenems, target the transpeptidase a… Show more

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Cited by 101 publications
(91 citation statements)
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References 17 publications
(39 reference statements)
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“…However, the lack of a Michaelis complex makes it difficult to decipher the exact role of R1 and R2 during the conformational rearrangements leading to acylation. A S. aureus PBP2a allosteric binding site has been inferred from kinetic studies, 50,62 and was recently supported by X-ray crystallography to be an 60 Å from the PBP2a TPase active site. 63 The allosteric site is located at the intersection of Lobe 1 (residues 166-240), Lobe 2 (residues 258-277), Lobe 3 (residues 364-390), and the N-terminal extension domain (residues 27-138).…”
mentioning
confidence: 88%
“…However, the lack of a Michaelis complex makes it difficult to decipher the exact role of R1 and R2 during the conformational rearrangements leading to acylation. A S. aureus PBP2a allosteric binding site has been inferred from kinetic studies, 50,62 and was recently supported by X-ray crystallography to be an 60 Å from the PBP2a TPase active site. 63 The allosteric site is located at the intersection of Lobe 1 (residues 166-240), Lobe 2 (residues 258-277), Lobe 3 (residues 364-390), and the N-terminal extension domain (residues 27-138).…”
mentioning
confidence: 88%
“…These strains may well represent heterogeneous groups, each with its own specific resistance mechanisms. Villegas-Estrada et al (61), using different determination and calculation methodology, tested the same (Hershey) VRSA strain examined in the current study as well as one different linezolid-resistant MRSA strain. Ceftaroline was found to be very active, with MICs of 0.25 to 2 g/ml.…”
Section: Vol 54 2010 Ceftaroline Affinity For Gram-positive Pbps 1671mentioning
confidence: 99%
“…Differences between our results and those reported previously (27) may be explained at least partially by differences in strains and culture conditions. The higher affinity of ceftaroline for PBP2a than those of other ␤-lactams may be explained by the presence of longer side chains in the chemical structure, which increase interactions with the active-site groove of PBP2a (6,37) and/or facilitate allosteric interactions that promote access to the active site (61). In MRSA strains, it is known that PBP2a may replace the transpeptidase function of PBP2, although the transglycosylase function of the latter becomes critical for MRSA growth in the presence of ␤-lactams (51).…”
Section: Vol 54 2010 Ceftaroline Affinity For Gram-positive Pbps 1671mentioning
confidence: 99%
“…Ceftaroline (CPT), the active metabolite of the prodrug CPTfosamil (CPT-F), demonstrates in vitro bactericidal activity against MRSA, including hVISA, VISA, and DNS strains (11)(12)(13)(14). Furthermore, some in vitro data suggest that CPT is more active against MRSA with reduced susceptibility to lipo-and glycopeptides than fully susceptible strains due to the phenomenon referred to as the "seesaw" effect (14)(15)(16).…”
mentioning
confidence: 99%