Zur Pharmakokinetik von Linezolid und Telithromycin: Zwei neue Antibiotika mit besonderen Eigenschaften

Sörgel, Fritz; Landersdorfer, Cornelia B.; Bulitta, Jürgen B.

doi:10.1002/pauz.200400052

Pharmazie in unserer Zeit

2004

DOI: 10.1002/pauz.200400052

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Zur Pharmakokinetik von Linezolid und Telithromycin: Zwei neue Antibiotika mit besonderen Eigenschaften

Fritz Sörgel

Cornelia B. Landersdorfer

Jürgen B. Bulitta

Abstract: Mit Linezolid und Telithromycin stehen zwei neue Antibiotika zur Verfügung, die sich in ihren pharmakokinetischen Eigenschaften von anderen Substanzklassen unterscheiden. Beim Linezolid fällt auf, dass es trotz seiner chemisch eher neutralen Eigenschaften sehr gut in Gewebe penetriert und ansonsten aufgrund seiner vollständigen oralen Resorption, seiner parenteralen Applizierbarkeit und seiner bisher nicht bekannten Neigung zu pharmakokinetischen Interaktionen eine gut überschaubare Substanz darstellt.Telithro… Show more

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2024

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Population pharmacokinetic rationale for intravenous contezolid acefosamil followed by oral contezolid dosage regimens

Bulitta,

Fang,

Stryjewski

et al. 2024

Antimicrob Agents Chemother

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Contezolid is a novel oxazolidinone antibiotic with a promising safety profile. Oral contezolid and its intravenous (IV) prodrug contezolid acefosamil (CZA) are in development for treatment of diabetic foot and acute bacterial skin and skin structure infections (ABSSSI). The prodrug CZA is converted to active contezolid via intermediate MRX-1352. This study aimed to provide the pharmacokinetic rationale for safe, effective, and flexible dosage regimens with initial IV CZA followed by oral contezolid. We simultaneously modeled plasma concentrations from 110 healthy volunteers and 74 phase 2 patients with ABSSSI via population pharmacokinetics (using the importance sampling estimation algorithm), and optimized dosage regimens by Monte Carlo simulations. This included data on MRX-1352, contezolid, and its metabolite MRX-1320 from 66 healthy volunteers receiving intravenous CZA (150–2400 mg) for up to 28 days, and 74 patients receiving oral contezolid [800 mg every 12 h (q12h)] for 10 days. The apparent total clearance for 800 mg oral contezolid with food was 16.0 L/h (23.4% coefficient of variation) in healthy volunteers and 17.7 L/h (53.8%) in patients. CZA was rapidly converted to MRX-1352, which subsequently transformed to contezolid. The proposed dosage regimen used an IV CZA 2000 mg loading dose with 1000 mg IV CZA q12h as maintenance dose(s), followed by 800 mg oral contezolid q12h (with food). During each 24-h period, Monte Carlo simulations predicted this regimen to achieve consistent areas under the curve of 91.9 mg·h/L (range: 76.3–106 mg·h/L) under all scenarios. Thus, this regimen was predicted to reliably achieve efficacious contezolid exposures independent of timing of switch from IV CZA to oral contezolid. IMPORTANCE This study provides the population pharmacokinetic rationale for the dosage regimen of the intravenous (IV) prodrug contezolid acefosamil (CZA) followed by oral contezolid. We developed the first integrated population model for the pharmacokinetics of the MRX-1352 intermediate prodrug, active contezolid, and its main metabolite MRX-1320 based on data from three clinical studies in healthy volunteers and phase 2 patients. The proposed regimen was predicted to reliably achieve efficacious contezolid exposures independent of timing of switch from IV CZA to oral contezolid.

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Population pharmacokinetic rationale for intravenous contezolid acefosamil followed by oral contezolid dosage regimens

Bulitta,

Fang,

Stryjewski

et al. 2024

Antimicrob Agents Chemother

View full text Add to dashboard Cite

show abstract

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Zur Pharmakokinetik von Linezolid und Telithromycin: Zwei neue Antibiotika mit besonderen Eigenschaften

Cited by 1 publication

References 20 publications

Population pharmacokinetic rationale for intravenous contezolid acefosamil followed by oral contezolid dosage regimens

Population pharmacokinetic rationale for intravenous contezolid acefosamil followed by oral contezolid dosage regimens

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