2007
DOI: 10.1128/aac.01533-06
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Concentration-Dependent Mycobacterium tuberculosis Killing and Prevention of Resistance by Rifampin

Abstract: Rifampin is a cornerstone of modern antituberculosis therapy. However, rifampin's half-life of 3 h is believed to limit its utility for intermittent therapy, so new congeners with long half-lives are being developed. Using an in vitro pharmacokinetic-pharmacodynamic model of tuberculosis, we examined the relationships between rifampin exposure, microbial killing of log-phase-growth Mycobacterium tuberculosis, and suppression of resistance. Rifampin's microbial killing was linked to the area under the concentra… Show more

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Cited by 315 publications
(315 citation statements)
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“…380,426,419 Table 11 shows the pharmacokineticpharmacodynamic exposure and pharmacokineticpharmacodynamic index associated with the sup pression of acquired drug resistance for several drugs that are used in clinical practice; these often differ from those associated with opti mal microbial kill for the same drug. 173,180,191,192,196,380,395,417,[419][420][421][422][423][424][425][426][427][428][429][430][431] Mistakenly, many regi mens were designed for the treatment of tuberculosis with a focus on microbial kill, ignoring the problem of acquired drug resistance. The theory was that directly observing the patients swallowing the pills, and using one drug to prevent resistance to another, would solve the acquired drug resistance problem.…”
Section: Pharmacokinetic-pharmacodynamic Indices and Microbial Kill Vmentioning
confidence: 99%
See 1 more Smart Citation
“…380,426,419 Table 11 shows the pharmacokineticpharmacodynamic exposure and pharmacokineticpharmacodynamic index associated with the sup pression of acquired drug resistance for several drugs that are used in clinical practice; these often differ from those associated with opti mal microbial kill for the same drug. 173,180,191,192,196,380,395,417,[419][420][421][422][423][424][425][426][427][428][429][430][431] Mistakenly, many regi mens were designed for the treatment of tuberculosis with a focus on microbial kill, ignoring the problem of acquired drug resistance. The theory was that directly observing the patients swallowing the pills, and using one drug to prevent resistance to another, would solve the acquired drug resistance problem.…”
Section: Pharmacokinetic-pharmacodynamic Indices and Microbial Kill Vmentioning
confidence: 99%
“…More data about drug exposure targets that would minimise therapy failure is available. Most data about acquired drug resistance was collected from preclinical models, 380,419,420,[426][427][428][429][430][431] except for one analysis of clinical studies in which all acquired drug resistance was preceded by low drug concentrations. 191,426 Drug concentrations are also likely to be lower than the optimal concentration in some anatomical compartments, such as the meninges and pericardial fluid, because of poor penetration of drugs into those compartments.…”
Section: Summary Of Pharmacokinetic-pharmacodynamic Factorsmentioning
confidence: 99%
“…Levels of rifampicin in the CSF are approximately 10-20% of those in plasma, depending on the severity of blood-brain barrier disruption [80]. The antimycobacterial activity of rifampicin is exposure-and concentration-dependent [81]. A relatively modest increase in administered doses of rifampicin (from 10mg/kg to 13 mg/kg) resulted in a significant increase (65%) in mean plasma area under the curve 0-24 h (AUC 0-24 h ) and 49% increase in plasma C max without a significant increase in the rate of adverse events [82,83].…”
Section: Specific Antituberculous Treatmentmentioning
confidence: 99%
“…20 Rifampicin was tested at 2 mg ml À1 , which represented a free peak concentration arising from a 600 mg, daily oral dose to maximize the use of the drug. 21 The concentrations of polymyxin B and tigecycline were tested at 0.5Â MIC to yield attainable experimental end points.…”
Section: Time-kill Studiesmentioning
confidence: 99%