The role of new posaconazole formulations in the treatment of candida albicans infections: Data from an in vitro Pharmacokinetic-Pharmacodynamic Model

Maria Ioanna Beredaki; Maiken Cavling Arendrup; David Andes; Johan W. Mouton; Joseph Meletiadis

doi:10.1128/AAC.01292-20

The role of new posaconazole formulations in the treatment of candida albicans infections: Data from an in vitro Pharmacokinetic-Pharmacodynamic Model

Maria Ioanna Beredaki, Maiken Cavling Arendrup, David Andes, Johan W. Mouton, Joseph Meletiadis

Research output: Contribution to journal › Journal article › Research › peer-review

12 Citations (Scopus)

Abstract

Posaconazole is more active than fluconazole against Candida albicans in vitro and is approved for the treatment of oropharyngeal candidiasis but not for that of invasive candidiasis (IC). Here, we explored the efficacy of posaconazole against C. albicans in an in vitro pharmacokinetic/pharmacodynamic (PK/PD) model of IC and determined the probability of pharmacodynamic target attainment for the oral solution and intravenous (i.v.)/tablet formulations. Three clinical C. albicans isolates (posaconazole MICs, 0.008 to 0.25 mg/liter) were studied in the in vitro PK/PD dilution model simulating steady-state posaconazole PK. The in vitro exposure-effect relationship, area under the 24-h free drug concentration curve (fAUC_0-24)/MIC, was described and compared with in vivo outcome in animals with IC. PK/PD susceptibility breakpoints and trough levels required for optimal treatment were determined for EUCAST and CLSI 24-h/48-h (CLSI24h/CLSI48h) methods using the fAUC_0-24/MIC associated with half-maximal activity (EI₅₀) and Monte Carlo simulation analysis for oral solution (400mg every 12 hours [q12h]) and i.v./tablet formulations (300mg q24h). The in vitro mean (95% confidence interval [CI]) EI50 was 330 (183 to 597) fAUC_0-24/MIC for CLSI24h and 169 (92 to 310) for EUCAST/CLSI48h methods, which are close to the near-stasis in vivo effect. The probability of target attainment for EI₅₀was estimated; for the wild-type isolates (MIC≤0.06 mg/liter), it was low for the oral solution and higher than 95% for the i.v./tablet formulations for the EUCAST/CLSI48h methods but not for the CLSI 24-h method. Non-wild-type isolates with EUCAST/ CLSI48h MICs of 0.125 and 0.25 mg/liter would require trough levels of >1.2 and >2.4 mg/liter, respectively. Posaconazole i.v./tablet formulations may have a role in the therapy of invasive infections by wild-type C. albicans isolates, provided that a steady state is reached quickly. A PK/PD susceptibility breakpoint at the epidemiological cutoff (ECV/ECOFF) of 0.06 mg/liter was determined.

Original language	English
Article number	e01292-20
Journal	Antimicrobial Agents and Chemotherapy
Volume	65
Issue number	4
ISSN	0066-4804
DOIs	https://doi.org/10.1128/AAC.01292-20
Publication status	Published - 2021

Keywords

breakpoints
Candida albicans
Candidiasis
CLSI
EUCAST
Monte Carlo simulation
Pharmacokineticpharmacodynamic
PK/PD susceptibility breakpoints
Posaconazole
Therapeutic drug monitoring

Access to Document

10.1128/AAC.01292-20

https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8097413/pdf/AAC.01292-20.pdfLicence: Other

Cite this

The role of new posaconazole formulations in the treatment of candida albicans infections : Data from an in vitro Pharmacokinetic-Pharmacodynamic Model. / Beredaki, Maria Ioanna; Arendrup, Maiken Cavling; Andes, David; Mouton, Johan W.; Meletiadis, Joseph.

In: Antimicrobial Agents and Chemotherapy, Vol. 65, No. 4, e01292-20, 2021.

Research output: Contribution to journal › Journal article › Research › peer-review

@article{b1b26351757b4281aadefabd3db4ace5,

title = "The role of new posaconazole formulations in the treatment of candida albicans infections: Data from an in vitro Pharmacokinetic-Pharmacodynamic Model",

abstract = "Posaconazole is more active than fluconazole against Candida albicans in vitro and is approved for the treatment of oropharyngeal candidiasis but not for that of invasive candidiasis (IC). Here, we explored the efficacy of posaconazole against C. albicans in an in vitro pharmacokinetic/pharmacodynamic (PK/PD) model of IC and determined the probability of pharmacodynamic target attainment for the oral solution and intravenous (i.v.)/tablet formulations. Three clinical C. albicans isolates (posaconazole MICs, 0.008 to 0.25 mg/liter) were studied in the in vitro PK/PD dilution model simulating steady-state posaconazole PK. The in vitro exposure-effect relationship, area under the 24-h free drug concentration curve (fAUC0-24)/MIC, was described and compared with in vivo outcome in animals with IC. PK/PD susceptibility breakpoints and trough levels required for optimal treatment were determined for EUCAST and CLSI 24-h/48-h (CLSI24h/CLSI48h) methods using the fAUC0-24/MIC associated with half-maximal activity (EI50) and Monte Carlo simulation analysis for oral solution (400mg every 12 hours [q12h]) and i.v./tablet formulations (300mg q24h). The in vitro mean (95% confidence interval [CI]) EI50 was 330 (183 to 597) fAUC0-24/MIC for CLSI24h and 169 (92 to 310) for EUCAST/CLSI48h methods, which are close to the near-stasis in vivo effect. The probability of target attainment for EI50was estimated; for the wild-type isolates (MIC≤0.06 mg/liter), it was low for the oral solution and higher than 95% for the i.v./tablet formulations for the EUCAST/CLSI48h methods but not for the CLSI 24-h method. Non-wild-type isolates with EUCAST/ CLSI48h MICs of 0.125 and 0.25 mg/liter would require trough levels of >1.2 and >2.4 mg/liter, respectively. Posaconazole i.v./tablet formulations may have a role in the therapy of invasive infections by wild-type C. albicans isolates, provided that a steady state is reached quickly. A PK/PD susceptibility breakpoint at the epidemiological cutoff (ECV/ECOFF) of 0.06 mg/liter was determined.",

keywords = "breakpoints, Candida albicans, Candidiasis, CLSI, EUCAST, Monte Carlo simulation, Pharmacokineticpharmacodynamic, PK/PD susceptibility breakpoints, Posaconazole, Therapeutic drug monitoring",

author = "Beredaki, {Maria Ioanna} and Arendrup, {Maiken Cavling} and David Andes and Mouton, {Johan W.} and Joseph Meletiadis",

year = "2021",

doi = "10.1128/AAC.01292-20",

language = "English",

volume = "65",

journal = "Antimicrobial Agents and Chemotherapy",

issn = "0066-4804",

publisher = "American Society for Microbiology",

number = "4",

}

TY - JOUR

T1 - The role of new posaconazole formulations in the treatment of candida albicans infections

T2 - Data from an in vitro Pharmacokinetic-Pharmacodynamic Model

AU - Beredaki, Maria Ioanna

AU - Arendrup, Maiken Cavling

AU - Andes, David

AU - Mouton, Johan W.

AU - Meletiadis, Joseph

PY - 2021

Y1 - 2021

N2 - Posaconazole is more active than fluconazole against Candida albicans in vitro and is approved for the treatment of oropharyngeal candidiasis but not for that of invasive candidiasis (IC). Here, we explored the efficacy of posaconazole against C. albicans in an in vitro pharmacokinetic/pharmacodynamic (PK/PD) model of IC and determined the probability of pharmacodynamic target attainment for the oral solution and intravenous (i.v.)/tablet formulations. Three clinical C. albicans isolates (posaconazole MICs, 0.008 to 0.25 mg/liter) were studied in the in vitro PK/PD dilution model simulating steady-state posaconazole PK. The in vitro exposure-effect relationship, area under the 24-h free drug concentration curve (fAUC0-24)/MIC, was described and compared with in vivo outcome in animals with IC. PK/PD susceptibility breakpoints and trough levels required for optimal treatment were determined for EUCAST and CLSI 24-h/48-h (CLSI24h/CLSI48h) methods using the fAUC0-24/MIC associated with half-maximal activity (EI50) and Monte Carlo simulation analysis for oral solution (400mg every 12 hours [q12h]) and i.v./tablet formulations (300mg q24h). The in vitro mean (95% confidence interval [CI]) EI50 was 330 (183 to 597) fAUC0-24/MIC for CLSI24h and 169 (92 to 310) for EUCAST/CLSI48h methods, which are close to the near-stasis in vivo effect. The probability of target attainment for EI50was estimated; for the wild-type isolates (MIC≤0.06 mg/liter), it was low for the oral solution and higher than 95% for the i.v./tablet formulations for the EUCAST/CLSI48h methods but not for the CLSI 24-h method. Non-wild-type isolates with EUCAST/ CLSI48h MICs of 0.125 and 0.25 mg/liter would require trough levels of >1.2 and >2.4 mg/liter, respectively. Posaconazole i.v./tablet formulations may have a role in the therapy of invasive infections by wild-type C. albicans isolates, provided that a steady state is reached quickly. A PK/PD susceptibility breakpoint at the epidemiological cutoff (ECV/ECOFF) of 0.06 mg/liter was determined.

AB - Posaconazole is more active than fluconazole against Candida albicans in vitro and is approved for the treatment of oropharyngeal candidiasis but not for that of invasive candidiasis (IC). Here, we explored the efficacy of posaconazole against C. albicans in an in vitro pharmacokinetic/pharmacodynamic (PK/PD) model of IC and determined the probability of pharmacodynamic target attainment for the oral solution and intravenous (i.v.)/tablet formulations. Three clinical C. albicans isolates (posaconazole MICs, 0.008 to 0.25 mg/liter) were studied in the in vitro PK/PD dilution model simulating steady-state posaconazole PK. The in vitro exposure-effect relationship, area under the 24-h free drug concentration curve (fAUC0-24)/MIC, was described and compared with in vivo outcome in animals with IC. PK/PD susceptibility breakpoints and trough levels required for optimal treatment were determined for EUCAST and CLSI 24-h/48-h (CLSI24h/CLSI48h) methods using the fAUC0-24/MIC associated with half-maximal activity (EI50) and Monte Carlo simulation analysis for oral solution (400mg every 12 hours [q12h]) and i.v./tablet formulations (300mg q24h). The in vitro mean (95% confidence interval [CI]) EI50 was 330 (183 to 597) fAUC0-24/MIC for CLSI24h and 169 (92 to 310) for EUCAST/CLSI48h methods, which are close to the near-stasis in vivo effect. The probability of target attainment for EI50was estimated; for the wild-type isolates (MIC≤0.06 mg/liter), it was low for the oral solution and higher than 95% for the i.v./tablet formulations for the EUCAST/CLSI48h methods but not for the CLSI 24-h method. Non-wild-type isolates with EUCAST/ CLSI48h MICs of 0.125 and 0.25 mg/liter would require trough levels of >1.2 and >2.4 mg/liter, respectively. Posaconazole i.v./tablet formulations may have a role in the therapy of invasive infections by wild-type C. albicans isolates, provided that a steady state is reached quickly. A PK/PD susceptibility breakpoint at the epidemiological cutoff (ECV/ECOFF) of 0.06 mg/liter was determined.

KW - breakpoints

KW - Candida albicans

KW - Candidiasis

KW - CLSI

KW - EUCAST

KW - Monte Carlo simulation

KW - Pharmacokineticpharmacodynamic

KW - PK/PD susceptibility breakpoints

KW - Posaconazole

KW - Therapeutic drug monitoring

U2 - 10.1128/AAC.01292-20

DO - 10.1128/AAC.01292-20

M3 - Journal article

C2 - 33468486

AN - SCOPUS:85102997005

VL - 65

JO - Antimicrobial Agents and Chemotherapy

JF - Antimicrobial Agents and Chemotherapy

SN - 0066-4804

IS - 4

M1 - e01292-20

ER -