Clinical Pharmacokinetics and Pharmacodynamics of Micafungin

Wasmann, Roeland E; Muilwijk, Eline W.; Burger, David M.; Verweij, Paul E.; Knibbe, Catherijne A. J.; Brüggemann, Roger J. M.

doi:10.1007/s40262-017-0578-5

Cited by 61 publications

(59 citation statements)

References 92 publications

(150 reference statements)

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“…A two-compartment model with first order elimination best described the micafungin plasma concentrations, which is in line with previous reports. 5,12,[18][19][20] In our study, body weight was the size descriptor best explaining the inter-individual variability in clearance, where individual clearance (in L/h) is predicted using the power function 0.69 * (weight / 70) 0.74 . This relation is supported by previously reported clearances in normal-weight healthy subjects.…”

Section: Discussionmentioning

confidence: 65%

“…Micafungin exhibits linear pharmacokinetics and is metabolized by arylsulfatase, catechol-Omethyltransferase and several cytochrome P450 (CYP) isoenzymes: CYP3A4, CYP1A2, CYP2B6 and CYP2C. 5 Pharmacokinetic (PK)-Pharmacodynamic (PD) targets for micafungin have been defined in patients with invasive candidiasis or candidemia based on the AUC over the MIC. For all Candida species excluding C. parapsilosis a breakpoint between 5,000 and 12,000 showed a 98% success rate in response versus 87% if patients had an AUC/MIC ratio below 5,000.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Pharmacokinetics and probability of target attainment for micafungin in normal-weight and morbidly obese adults

Wasmann

Smit

Heine³

et al. 2019

Journal of Antimicrobial Chemotherapy

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Objectives. The rising pandemic of obesity makes that more obese patients with serious infections require antimicrobial therapy. Micafungin is an echinocandin drug frequently used as therapy or prophylaxis of fungal infections, predominantly with Candida species. In order to maximize efficacy of micafungin in obese patients, the dose that corresponds with optimal exposure for each obese individual needs to be identified. Methods. We performed a prospective study in sixteen obese and eight normal-weight healthy subjects with a weight ranging 61.5 to 184 kg (ClinicalTrials.gov Identifier: NCT03102658). A population pharmacokinetic model was developed and used to simulate several dosing regimens to evaluate the PTA for relevant MICs to define the optimal dose using the PK-PD target of an AUC/MIC ratio above 5,000. Results. Total body weight was found to be most predictive for clearance and volume of distribution. Simulations show that a 100 mg dose results in a PTA above 90% in patients up to 125 kg with an MIC of 0.016 mg/L. The maintenance dose should be increased to 200 mg in patients above 125 kg infected with a Candida species with an MIC of 0.016 mg/L. At an MIC of 0.032 mg/L, a 300 mg maintenance dose is recommended above 125 kg weight. Furthermore, we demonstrate that patients can benefit from a loading dose (i.e. twice the maintenance dose). Conclusions. We present easy-to-use dose recommendations for obese patients based on both weight and target MIC that results in adequate exposure in patients with body weights up to 190 kg.

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Section: Discussionmentioning

confidence: 65%

Section: Introductionmentioning

confidence: 99%

Pharmacokinetics and probability of target attainment for micafungin in normal-weight and morbidly obese adults

Wasmann

Smit

Heine³

et al. 2019

Journal of Antimicrobial Chemotherapy

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“…Structural and chemical similarities (e.g., lipophilicity) of posaconazole to itraconazole, and high protein binding of posaconazole (>98%) and echinocandins (84-99.85%) (Hajdu et al, 1997;Paderu et al, 2007;Felton et al, 2014;Wasmann et al, 2018) may allow speculation for poor saliva penetration of these drugs.…”

Section: Discussionmentioning

confidence: 99%

Saliva for Precision Dosing of Antifungal Drugs: Saliva Population PK Model for Voriconazole Based on a Systematic Review.

et al. 2020

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Precision dosing for many antifungal drugs is now recommended. Saliva sampling is considered as a non-invasive alternative to plasma sampling for therapeutic drug monitoring (TDM). However, there are currently no clinically validated saliva models available. The aim of this study is firstly, to conduct a systematic review to evaluate the evidence supporting saliva-based TDM for azoles, echinocandins, amphotericin B, and flucytosine. The second aim is to develop a saliva population pharmacokinetic (PK) model for eligible drugs, based on the evidence. Databases were searched up to July 2019 on PubMed ® and Embase ® , and 14 studies were included in the systematic review for fluconazole, voriconazole, itraconazole, and ketoconazole. No studies were identified for isavuconazole, posaconazole, flucytosine, amphotericin B, caspofungin, micafungin, or anidulafungin. Fluconazole and voriconazole demonstrated a good saliva penetration with an average S/P ratio of 1.21 (± 0.31) for fluconazole and 0.56 (± 0.18) for voriconazole, both with strong correlation (r = 0.89-0.98). Based on the evidence for TDM and available data, population PK analysis was performed on voriconazole using Nonlinear Mixed Effects Modeling (NONMEM 7.4). 137 voriconazole plasma and saliva concentrations from 11 patients (10 adults, 1 child) were obtained from the authors of the included study. Voriconazole pharmacokinetics was best described by one-compartment PK model with first-order absorption, parameterized by clearance of 4.56 L/h (36.9% CV), volume of distribution of 60.7 L, absorption rate constant of 0.858 (fixed), and bioavailability of 0.849. Kinetics of the voriconazole distribution from plasma to saliva was identical to the plasma kinetics, but the extent of distribution was lower, modeled by a scale factor of 0.5 (4% CV). A proportional error model best accounted for the residual variability. The visual and simulation-based model diagnostics confirmed a good predictive performance of the

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“…Micafungin has a low hepatic extraction ratio with high protein binding in plasma, and while its total plasma concentration may decrease in some clinical cases, the unbound fraction of the drug is likely to remain stable [151,152]. A phase I parallel group open-label PK study of a single-dose of micafungin included 8 patients with Child–Pugh Score 7–9 hepatic dysfunction and did not find significant difference in unbound plasma concentration of the drug compared with healthy controls, while a lower AUC was found in the patients with hepatic impairment [153].…”

Section: Antifungal Agentsmentioning

confidence: 99%

Pre-Existing Liver Disease and Toxicity of Antifungals

Spernovasilis

Kofteridis

2018

JoF

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Pre-existing liver disease in patients with invasive fungal infections further complicates their management. Altered pharmacokinetics and tolerance issues of antifungal drugs are important concerns. Adjustment of the dosage of antifungal agents in these cases can be challenging given that current evidence to guide decision-making is limited. This comprehensive review aims to evaluate the existing evidence related to antifungal treatment in individuals with liver dysfunction. This article also provides suggestions for dosage adjustment of antifungal drugs in patients with varying degrees of hepatic impairment, after accounting for established or emerging pharmacokinetic–pharmacodynamic relationships with regard to antifungal drug efficacy in vivo.

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Clinical Pharmacokinetics and Pharmacodynamics of Micafungin

Cited by 61 publications

References 92 publications

Pharmacokinetics and probability of target attainment for micafungin in normal-weight and morbidly obese adults

Pharmacokinetics and probability of target attainment for micafungin in normal-weight and morbidly obese adults

Saliva for Precision Dosing of Antifungal Drugs: Saliva Population PK Model for Voriconazole Based on a Systematic Review.

Pre-Existing Liver Disease and Toxicity of Antifungals

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