Cellular Pharmacokinetics of the Novel Biaryloxazolidinone Radezolid in Phagocytic Cells: Studies with Macrophages and Polymorphonuclear Neutrophils

Lemaire, Sandrine; Tulkens, Paul M.; Bambeke, Françoise Van

doi:10.1128/aac.01723-09

Cited by 64 publications

(58 citation statements)

References 49 publications

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“…It is also interesting to note that both moxifloxacin and delafloxacin are found in the soluble fraction of the cells, with only a minimal amount detected in the organelles, as already observed for other fluoroquinolones (12,41). This is in opposition to what is seen with weak bases like macrolides or the biaryloxazolidinone radezolid, which are associated in large proportion with acidic vacuoles such as lysosomes (13,25). While such molecules show a marked decrease of accumulation when the pH gradient between subcellular compartments and the extracellular milieu is collapsed with monensin (25), the weak acid character of delafloxacin results in an opposite behavior.…”

Section: Discussioncontrasting

confidence: 46%

“…This is in opposition to what is seen with weak bases like macrolides or the biaryloxazolidinone radezolid, which are associated in large proportion with acidic vacuoles such as lysosomes (13,25). While such molecules show a marked decrease of accumulation when the pH gradient between subcellular compartments and the extracellular milieu is collapsed with monensin (25), the weak acid character of delafloxacin results in an opposite behavior. Moxifloxacin behaves similarly to the weak bases in this respect, probably due to the presence of a protonatable amino group.…”

Section: Discussioncontrasting

confidence: 44%

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Contrasting Effects of Acidic pH on the Extracellular and Intracellular Activities of the Anti-Gram-Positive Fluoroquinolones Moxifloxacin and Delafloxacin againstStaphylococcus aureus

Lemaire

Tulkens

Bambeke

2011

Antimicrob Agents Chemother

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166

140

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In contrast to currently marketed fluoroquinolones, which are zwitterionic, delafloxacin is an investigational fluoroquinolone with an anionic character that is highly active against Gram-positive bacteria. We have examined the effect of acidic pH on its accumulation in Staphylococcus aureus and in human THP-1 cells, in parallel with its activity against extracellular and intracellular S. aureus. Moxifloxacin was used as a comparator. Delafloxacin showed MICs 3 to 5 log 2 dilutions lower than those of moxifloxacin for a collection of 35 strains with relevant resistance mechanisms and also proved to be 10-fold more potent against intracellular S. aureus ATCC 25923. In medium at pH 5.5, this difference was further enhanced, with the MIC decreasing by 5 log 2 dilutions. In infected cells incubated in acidic medium, the relative potency was 10-fold higher than that at neutral pH and the maximal relative efficacy reached a bactericidal effect at 24 h. These results can be explained by a 10-fold increase in delafloxacin accumulation in both bacteria and cells at acidic pH, making delafloxacin one of the most efficient drugs tested in this model. Opposite effects were seen for moxifloxacin with respect to both activity and accumulation. As reported for zwitterionic fluoroquinolones, delafloxacin was found associated with the soluble fraction in homogenates of eukaryotic cells. Taken together, these properties may confer to delafloxacin an advantage for the eradication of S. aureus in acidic environments, including intracellular infections.Fluoroquinolones are one of the first families of fully synthetic antibiotics with large clinical use, and they represent a wide range of molecules, which permits the establishment of in-depth structure-activity relationships (16,17). Over the last 20 years, most fluoroquinolone research efforts have been focused on new molecules with improved activity toward Grampositive cocci because of the increasing spread of multiresistant staphylococci and streptococci. The 8-methoxy fluoroquinolone moxifloxacin is the first example of this new generation to reach the commercial market. It combines many desirable microbiological and pharmacokinetic properties (rapid bactericidal activity, a spectrum covering pertinent pathogens, excellent oral bioavailability, a large tissue distribution, and a propensity to accumulate within eukaryotic cells [see reference 45 for a review]). Moxifloxacin shows extensive activity toward bacteria thriving in the cytosol (Listeria monocytogenes [14]), phagosomes (Legionella pneumophila, Mycobacterium avium, and Mycobacterium tuberculosis [5,9,46]), and phagolysosomes (Staphylococcus aureus [6]), suggesting that it easily diffuses between different subcellular compartments. Yet moxifloxacin activity is partially defeated by the acidic pH prevailing in vacuolar subcellular compartments (6).Delafloxacin [RX-3341; 1-(6-amino-3,5-difluoropyridin-2-yl)-8-chloro-6-fluoro-7-(3-hydroxyazetidin-1-yl)-4-oxo-1,4-dihydroquinoline-3-carboxylic acid] is an investigational fluoro...

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Section: Discussioncontrasting

confidence: 46%

Section: Discussioncontrasting

confidence: 44%

Contrasting Effects of Acidic pH on the Extracellular and Intracellular Activities of the Anti-Gram-Positive Fluoroquinolones Moxifloxacin and Delafloxacin againstStaphylococcus aureus

Lemaire

Tulkens

Bambeke

2011

Antimicrob Agents Chemother

Self Cite

166

140

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“…It displayed MIC 90 values against cfr-containing linezolid-resistant S. aureus isolates that were 4-to 8-fold lower than those of linezolid (103). Another attractive property of this compound is higher intrinsic activity than linezolid in infected cells, with phagocytic cell internal concentrations increased 11-fold over extracellular concentrations (104,105). The compound has recently successfully completed two phase 2 clinical trials for community-acquired pneumonia (CAP) and for uncomplicated skin and skin structure infections (uSSSI) (http://www.clinicaltrials.gov).…”

Section: Oxazolidinonesmentioning

confidence: 99%

Investigational Antimicrobial Agents of 2013

Pucci

Bush

2013

Clin Microbiol Rev

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SUMMARY New antimicrobial agents are always needed to counteract the resistant pathogens that continue to be selected by current therapeutic regimens. This review provides a survey of known antimicrobial agents that were currently in clinical development in the fall of 2012 and spring of 2013. Data were collected from published literature primarily from 2010 to 2012, meeting abstracts (2011 to 2012), government websites, and company websites when appropriate. Compared to what was reported in previous surveys, a surprising number of new agents are currently in company pipelines, particularly in phase 3 clinical development. Familiar antibacterial classes of the quinolones, tetracyclines, oxazolidinones, glycopeptides, and cephalosporins are represented by entities with enhanced antimicrobial or pharmacological properties. More importantly, compounds of novel chemical structures targeting bacterial pathways not previously exploited are under development. Some of the most promising compounds include novel β-lactamase inhibitor combinations that target many multidrug-resistant Gram-negative bacteria, a critical medical need. Although new antimicrobial agents will continue to be needed to address increasing antibiotic resistance, there are novel agents in development to tackle at least some of the more worrisome pathogens in the current nosocomial setting.

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“…Cell fractionation and subcellular localization studies were therefore conducted to determine whether intracellular tedizolid would be associated with mitochondria, which might represent a possible toxicity hazard. Murine J774 macrophages were selected because these cells can easily be fractionated and their mitochondria adequately separated from other cell organelles by centrifugation (39). The methods were previously described in detail and validated to determine the subcellular localization of various antibiotics, such as aminoglycosides, fluoroquinolones, and macrolides (40) as well as oxazolidinones (39).…”

Section: Methodsmentioning

confidence: 99%

“…Murine J774 macrophages were selected because these cells can easily be fractionated and their mitochondria adequately separated from other cell organelles by centrifugation (39). The methods were previously described in detail and validated to determine the subcellular localization of various antibiotics, such as aminoglycosides, fluoroquinolones, and macrolides (40) as well as oxazolidinones (39). Cells were incubated for 2 h with 20 mg/liter tedizolid before collection.…”

Section: Methodsmentioning

confidence: 99%

Nonclinical and Pharmacokinetic Assessments To Evaluate the Potential of Tedizolid and Linezolid To Affect Mitochondrial Function

Flanagan

McKee

Das

et al. 2015

Antimicrob Agents Chemother

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e Prolonged treatment with the oxazolidinone linezolid is associated with myelosuppression, lactic acidosis, and neuropathies, toxicities likely caused by impairment of mitochondrial protein synthesis (MPS). To evaluate the potential of the novel oxazolidinone tedizolid to cause similar side effects, nonclinical and pharmacokinetic assessments were conducted. In isolated rat heart mitochondria, tedizolid inhibited MPS more potently than did linezolid (average [؎ standard error of the mean] 50% inhibitory concentration [IC 50 ] for MPS of 0.31 ؎ 0.02 M versus 6.4 ؎ 1.2 M). However, a rigorous 9-month rat study comparing placebo and high-dose tedizolid (resulting in steady-state area under the plasma concentration-time curve values about 8-fold greater than those with the standard therapeutic dose in humans) showed no evidence of neuropathy. Additional studies explored why prolonged, high-dose tedizolid did not cause these mitochondriopathic side effects despite potent MPS inhibition by tedizolid. Murine macrophage (J774) cell fractionation studies found no evidence of a stable association of tedizolid with eukaryotic mitochondria. Monte Carlo simulations based on population pharmacokinetic models showed that over the course of a dosing interval using standard therapeutic doses, free plasma concentrations fell below the respective MPS IC 50 in 84% of tedizolid-treated patients (for a median duration of 7.94 h) and 38% of linezolid-treated patients (for a median duration of 0 h). Therapeutic doses of tedizolid, but not linezolid, may therefore allow for mitochondrial recovery during antibacterial therapy. The overall results suggest that tedizolid has less potential to cause myelosuppression and neuropathy than that of linezolid during prolonged treatment courses. This, however, remains a hypothesis that must be confirmed in clinical studies.

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Cellular Pharmacokinetics of the Novel Biaryloxazolidinone Radezolid in Phagocytic Cells: Studies with Macrophages and Polymorphonuclear Neutrophils

Cited by 64 publications

References 49 publications

Contrasting Effects of Acidic pH on the Extracellular and Intracellular Activities of the Anti-Gram-Positive Fluoroquinolones Moxifloxacin and Delafloxacin againstStaphylococcus aureus

Contrasting Effects of Acidic pH on the Extracellular and Intracellular Activities of the Anti-Gram-Positive Fluoroquinolones Moxifloxacin and Delafloxacin againstStaphylococcus aureus

Investigational Antimicrobial Agents of 2013

Nonclinical and Pharmacokinetic Assessments To Evaluate the Potential of Tedizolid and Linezolid To Affect Mitochondrial Function

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