Clinical Role of Protein Binding of Quinolones

Bergogne-Bérézin, E

doi:10.2165/00003088-200241100-00004

Cited by 76 publications

(66 citation statements)

References 39 publications

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“…Most fluoroquinolones are moderately lipophilic drugs with a molecular mass of around 300 Da and low binding to plasma proteins (approximately 20 to 40%) (21). Around the physiological pH, most agents are uncharged, which favors their CNS penetration.…”

Section: Fluoroquinolonesmentioning

confidence: 99%

Penetration of Drugs through the Blood-Cerebrospinal Fluid/Blood-Brain Barrier for Treatment of Central Nervous System Infections

2010

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SUMMARY The entry of anti-infectives into the central nervous system (CNS) depends on the compartment studied, molecular size, electric charge, lipophilicity, plasma protein binding, affinity to active transport systems at the blood-brain/blood-cerebrospinal fluid (CSF) barrier, and host factors such as meningeal inflammation and CSF flow. Since concentrations in microdialysates and abscesses are not frequently available for humans, this review focuses on drug CSF concentrations. The ideal compound to treat CNS infections is of small molecular size, is moderately lipophilic, has a low level of plasma protein binding, has a volume of distribution of around 1 liter/kg, and is not a strong ligand of an efflux pump at the blood-brain or blood-CSF barrier. When several equally active compounds are available, a drug which comes close to these physicochemical and pharmacokinetic properties should be preferred. Several anti-infectives (e.g., isoniazid, pyrazinamide, linezolid, metronidazole, fluconazole, and some fluoroquinolones) reach a CSF-to-serum ratio of the areas under the curves close to 1.0 and, therefore, are extremely valuable for the treatment of CNS infections. In many cases, however, pharmacokinetics have to be balanced against in vitro activity. Direct injection of drugs, which do not readily penetrate into the CNS, into the ventricular or lumbar CSF is indicated when other effective therapeutic options are unavailable.

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Section: Fluoroquinolonesmentioning

confidence: 99%

Penetration of Drugs through the Blood-Cerebrospinal Fluid/Blood-Brain Barrier for Treatment of Central Nervous System Infections

2010

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“…For example, protein binding of clarithromycin may be as low as of 42 to 50% over a concentration range of 0.25 to 0.5 mg/L [54], or as high as 72% over a concentration range of 0.04 to 1.0 mg/L [55,56]. Protein binding of moxifloxacin being concentration independent was found to range from 25% [57] to 52% [58]. Such differences really matter, as the free fraction used as basis for PK/PD calculations could be assumed to be as low as 30% and 48% or as high as 60% and 75%, respectively.…”

Section: Discussionmentioning

confidence: 99%

The Impact of Protein Binding on Antibacterial Activities of Antibiotics is more than Predicted by Considering its Numerical Value Alone: Impact of Preparative and Incubation Methods on Different Pharmacodynamic Endpoints of ß-Lactams, Macrolides, or Fluoroquinolones Against Gram-positive and Gram-negative Bacteria-Part I

Dalhoff¹,

Schubert²

2016

J Clin Infect Dis Pract

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Objectives: Protein binding decreases antibacterial activities as the free fraction only crosses membranes thus reaching intracellular targets. However, serum components may also increase antibacterial activities. Therefore, the effect of serum proteins on activities of ß-lactams, macrolides, and fluoroquinolones was examined. Several preparation-and cultivation-conditions were examined as some preparative methods like freeze-thawing of sera may cause artifacts. Furthermore, previous studies have indicated that data may vary depending on the endpoints studied. Therefore, the aim of this study was to avoid an impact of methodological factors on the data generated and to analyse the activities of the study drugs by examining different static-or dynamic endpoints.Methods: Bacteria were grown in Brain Heart Infusion Broth (BHI), plus 50% of either fresh inactivated, pH 7.2, or fresh inactivated-, pH 7.2 or 8.2, frozen inactivated-serum, pH 8.2 as compared to BHI without any supplementations, pH 7.2 or 8.2, and BHI plus 45 g/L albumin. MICs of faropenem, amoxicillin, clarithromycin, azithromycin, moxifloxacin, and levofloxacin were determined and kill-kinetics were recorded following exposure to constant or fluctuating drug concentrations simulating serum pharmacokinetics of the agents. Kill-rates and areas under the bacterial kill curves were calculated.Results: Albumin and inactive serum increased MICs and reduced kill-rates of the agents studied in conformity with their protein binding, whereas active serum increased the activities of the agents. MICs and kill-rates did not change in parallel. The impact of protein binding in decreasing order was: MICs>kill-rates in time-kill experiments>kill-rates in kinetic-simulations. Macrolides and fluoroquinolones but not ß-lactams were more active at an alkaline-than neutral pH. Use of frozen sera caused alkalinization of media, thus generating artifacts. Conclusions:The impact of serum proteins on antibacterial activities is strongly dependent from three factors: the methods applied to prepare the serum pool, the incubation conditions, and the enpoints studied.

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“…The relevance of PB on PKs and the microbiological efficacy of an antibiotic were considered clinically important in case of highly bound agents (17). It is well-established that only the protein unbound fraction of a drug in plasma can readily penetrate into and equilibrate with the extravascular space (3). Sufficient tissue penetration of drugs is, in turn, a prerequisite for successful treatment of the majority of bacterial infections, which occur in the interstitial fluid (ISF) rather than in the blood (18).…”

Section: Principles Of Plasma Protein Binding Of Antibioticsmentioning

confidence: 99%

“…In contrast, no general consensus has been reached, whether PB also pharmacodynamically impacts antimicrobial activity by reducing the free, i.e., nonprotein-bound, fraction of an antibiotic (3,4). The unfavorable effect of PB on bacterial killing is generally accepted for β-lactams (5,6), whereas doubts about the usefulness of extrapolation of findings from β-lactams to other antimicrobial classes, such as fluoroquinolones, persist (3,4). There is currently no standardization of in vitro pharmacodynamic (PD) models, which account for the impact of PB of antimicrobials (7).…”

Section: Introductionmentioning

confidence: 99%

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Protein Binding of Antimicrobials: Methods for Quantification and for Investigation of its Impact on Bacterial Killing

Beer

Wagner

Zeitlinger

2009

AAPS J

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Abstract. Plasma protein binding of antimicrobial agents is considered to be a key characteristic of antibiotics as it affects both their pharmacokinetics and pharmacodynamics. However, up to the present, no standard methods for measuring protein binding or for quantification of the influence of protein binding on antimicrobial activity exist. This short-coming has previously led to conflicting results on antibacterial activity of highly protein-bound antibiotics. The present review, therefore, set out to summarize (1) methods for quantification of protein binding, (2) microbiological growth media used for determination of the impact of protein binding on antimicrobial activity of antibiotics, and (3) different pharmacodynamic in vitro studies that are used in this context. The advantages and disadvantages of a wide range of different approaches are discussed and compared. The urgent call for international standardization by microbiological societies and laboratories may be considered as a logical consequence of the presented data.

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Clinical Role of Protein Binding of Quinolones

Cited by 76 publications

References 39 publications

Penetration of Drugs through the Blood-Cerebrospinal Fluid/Blood-Brain Barrier for Treatment of Central Nervous System Infections

Penetration of Drugs through the Blood-Cerebrospinal Fluid/Blood-Brain Barrier for Treatment of Central Nervous System Infections

Protein Binding of Antimicrobials: Methods for Quantification and for Investigation of its Impact on Bacterial Killing

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