Therapeutic Drug Monitoring of Antifungal Drugs: Another Tool to Improve Patient Outcome?

Vena, Antonio; Mateos, Miriam; Guinea, Jesús; Galar, Alicia; Pea, Federico; Álvarez‐Uría, Ana; Escribano, Pilar; Bouza, Emilio

doi:10.1007/s40121-020-00280-y

Cited by 32 publications

(21 citation statements)

References 52 publications

(94 reference statements)

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“…Collectively, these data indicate the predictive potential of FLZ MIC ≥ 32 µg/mL for FLZ TF and of FKS sequencing combined with AFST data for echinocandin TF. However, it should be noted that TF cannot be exclusively attributed to microbiological characteristics of the isolates; other factors may be involved, including serum concentration of the antifungal which shows patient‐to‐patient variations, highlighting the importance of therapeutic drug monitoring to attain a favourable clinical outcome 58 . Moreover, considering that all patients with azole/echinocandin‐resistant C glabrata isolates had a catheter inserted (except one patient infected with isolate #G6 without clinical data), it is plausible that catheter removal may have implications on clinical outcome.…”

Section: Resultsmentioning

confidence: 99%

Low level of antifungal resistance of Candida glabrata blood isolates in Turkey: Fluconazole minimum inhibitory concentration and FKS mutations can predict therapeutic failure

Arastehfar

Daneshnia²,

Salehi

et al. 2020

Mycoses

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Background Candida glabrata is the third leading cause of candidaemia in Turkey; however, the data regarding antifungal resistance mechanisms and genotypic diversity in association with their clinical implication are limited. Objectives To assess genotypic diversity, antifungal susceptibility and mechanisms of drug resistance of C glabrata blood isolates and their association with patients' outcome in a retrospective multicentre study. Patients/Methods Isolates from 107 patients were identified by ITS sequencing and analysed by multilocus microsatellite typing, antifungal susceptibility testing, and sequencing of PDR1 and FKS1/2 hotspots (HSs). Results Candida glabrata prevalence in Ege University Hospital was twofold higher in 2014‐2019 than in 2005‐2014. Six of the analysed isolates had fluconazole MICs ≥ 32 µg/mL; of them, five harboured unique PDR1 mutations. Although echinocandin resistance was not detected, three isolates had mutations in HS1‐Fks1 (S629T, n = 1) and HS1‐Fks2 (S663P, n = 2); one of the latter was also fluconazole‐resistant. All patients infected with isolates carrying HS‐FKS mutations and/or demonstrating fluconazole MIC ≥ 32 µg/mL (except one without clinical data) showed therapeutic failure (TF) with echinocandin and fluconazole; seven such isolates were collected in Ege (n = 4) and Gulhane (n = 3) hospitals and six detected recently. Among 34 identified genotypes, none were associated with mortality or enriched for fluconazole‐resistant isolates. Conclusion Antifungal susceptibility testing should be supplemented with HS‐FKS sequencing to predict TF for echinocandins, whereas fluconazole MIC ≥ 32 µg/mL may predict TF. Recent emergence of C glabrata isolates associated with antifungal TF warrants future comprehensive prospective studies in Turkey.

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Section: Resultsmentioning

confidence: 99%

Low level of antifungal resistance of Candida glabrata blood isolates in Turkey: Fluconazole minimum inhibitory concentration and FKS mutations can predict therapeutic failure

Arastehfar

Daneshnia²,

Salehi

et al. 2020

Mycoses

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“…When used in critically ill patients, voriconazole demonstrated a large inter-patient variability in voriconazole plasma concentrations ranging from ≤ 1 mg/L for 37% of patients to > 5.5 mg/L for 19% of them [ 4 ]. Moreover, sub-therapeutic triazoles concentrations including voriconazole were linked to poor outcome compared with optimal concentrations [ 5 , 6 ], whereas voriconazole supra-therapeutic concentrations were identified as a significant independent risk factor for hepatotoxicity in critically ill patients [ 7 , 8 ]. Thus, voriconazole TDM is needed in critically ill patients to improve efficacy and safety as recently demonstrated [ 9 ].…”

Section: Introductionmentioning

confidence: 99%

Association between voriconazole exposure and Sequential Organ Failure Assessment (SOFA) score in critically ill patients

et al. 2021

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Therapeutic drug monitoring (TDM) is essential for voriconazole to ensure optimal drug exposure, mainly in critically ill patients for whom voriconazole demonstrated a large variability. The study aimed at describing factors associated with trough voriconazole concentrations in critically ill patients and evaluating the impact of voriconazole concentrations on adverse effects. A 2-year retrospective multicenter cohort study (NCT04502771) was conducted in six intensive care units. Adult patients who had at least one voriconazole TDM were included. Univariable and multivariable linear regression analyses were performed to identify predictors of voriconazole concentrations, and univariable logistic regression analysis, to study the relationship between voriconazole concentrations and adverse effects. During the 2-year study period, 70 patients were included. Optimal trough voriconazole concentrations were reported in 37 patients (52.8%), subtherapeutic in 20 (28.6%), and supratherapeutic in 13 (18.6%). Adverse effects were reported in six (8.6%) patients. SOFA score was identified as a factor associated with an increase in voriconazole concentration (p = 0.025), mainly in the group of patients who had SOFA score ≥ 10. Moreover, an increase in voriconazole concentration was shown to be a risk factor for occurrence of adverse effects (p = 0.011). In that respect, critically ill patients who received voriconazole treatment must benefit from a TDM, particularly if they have a SOFA score ≥ 10. Indeed, identifying patients who are overdosed will help to prevent voriconazole related adverse effects. This result is of utmost importance given the recognized COVID-19-associated pulmonary aspergillosis in ICU patients for whom voriconazole is among the recommended first-line treatment.

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“…Future development axes to improve the prognosis would involve new laboratory diagnostic and imaging procedures and the search for new antifungal compounds. In any case, drug monitoring should be a preliminary to any antifungal treatment because a large proportion of patients exhibit low drug concentrations leading to poor outcomes, especially in ICU settings [ 37 ].…”

Section: Discussionmentioning

confidence: 99%

Emerging Invasive Fungal Infections in Critically Ill Patients: Incidence, Outcomes and Prognosis Factors, a Case-Control Study

Larcher

Platon²,

Brunot³

et al. 2021

JoF

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Comprehensive data on emerging invasive fungal infections (EIFIs) in the critically ill are scarce. We conducted a case-control study to characterize EIFIs in patients admitted to a French medical ICU teaching hospital from 2006 to 2019. Among 6900 patients, 26 (4 per 1000) had an EIFI: Mucorales accounted for half, and other isolates were mainly Saprochaete, Fusarium and Scedosporium. EIFIs occurred mostly in patients with immunosuppression and severe critical illness. Antifungal treatments (mainly amphotericin B) were administered to almost all patients, whereas only 19% had surgery. In-ICU, mortality was high (77%) and associated with previous conditions such as hematological malignancy or cancer, malnutrition, chronic kidney disease and occurrence of acute respiratory distress syndrome and/or hepatic dysfunction. Day-90 survival rates, calculated by the Kaplan–Meier method, were similar between patients with EIFIs and a control group of patients with aspergillosis: 20%, 95% CI (9- 45) versus 18%, 95% CI (8- 45) (log-rank: p > 0.99). ICU management of such patients should be assessed on the basis of underlying conditions, reversibility and acute event severity rather than the mold species.

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Therapeutic Drug Monitoring of Antifungal Drugs: Another Tool to Improve Patient Outcome?

Cited by 32 publications

References 52 publications

Low level of antifungal resistance of Candida glabrata blood isolates in Turkey: Fluconazole minimum inhibitory concentration and FKS mutations can predict therapeutic failure

Low level of antifungal resistance of Candida glabrata blood isolates in Turkey: Fluconazole minimum inhibitory concentration and FKS mutations can predict therapeutic failure

Association between voriconazole exposure and Sequential Organ Failure Assessment (SOFA) score in critically ill patients

Emerging Invasive Fungal Infections in Critically Ill Patients: Incidence, Outcomes and Prognosis Factors, a Case-Control Study

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