2012
DOI: 10.1126/scitranslmed.3003592
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Restoring Methicillin-Resistant Staphylococcus aureus Susceptibility to β-Lactam Antibiotics

Abstract: Methicillin-resistant Staphylococcus aureus infection can be treated effectively by combining a β-lactam antibiotic with a drug that targets FtsZ.

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Cited by 212 publications
(308 citation statements)
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“…. The yellow-colored molecule is PC190723, which is located at the interdomain cleft between H7 helix and C-terminal domain (PDB entry 4DXD) [25].…”
Section: The Structurementioning
confidence: 99%
See 3 more Smart Citations
“…. The yellow-colored molecule is PC190723, which is located at the interdomain cleft between H7 helix and C-terminal domain (PDB entry 4DXD) [25].…”
Section: The Structurementioning
confidence: 99%
“…The t 1/2 of TXA707 following intravenous administration of TXA709 was 3.65 h, while the t 1/2 of PC190723 following the intravenous administration of TXA541 was 0.56 h. TXA709 thus displayed better pharmacokinetic properties by keeping its strong antibacterial activity and its efficacy in vivo. In a study of the mice model infected with MRSA ATCC 33591, a 2-log reduction in bacterial CFU can be found in the model treated with 120 or 160 mg kg −1 of TXA709 administered orally, while only about 0.5-log reduction was found when orally administered 200 mg kg −1 of PC190723 [25,97]. …”
Section: Dichamanetin and Its Derivativementioning
confidence: 99%
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“…However, the robustness of the MRSA phenotype is modulated by many other aspects of the MSSA strain background that acquires mecA (6). The complexity of the MRSA phenotype thus offers hope that drug interactions and other interventions can be devised that will allow the restoration of an MSSA phenotype to MRSA strains (7)(8)(9). The work of Brown et al (4) identifies a significant target that may be exploited to allow resensitization of MRSA.…”
mentioning
confidence: 99%