Your search keyword '"Esteve-Pitarch, Erika"' showing total 2 results

1. A Real-World Data Observational Analysis of the Impact of Liposomal Amphotericin B on Renal Function Using Machine Learning in Critically Ill Patients.

Author

Sacanella, Ignasi, Esteve-Pitarch, Erika, Guevara-Chaux, Jessica, Berrueta, Julen, García-Martínez, Alejandro, Gómez, Josep, Casarino, Cecilia, Alés, Florencia, Canadell, Laura, Martín-Loeches, Ignacio, Grau, Santiago, Candel, Francisco Javier, Bodí, María, and Rodríguez, Alejandro

Subjects

ANTIFUNGAL agents, AMPHOTERICIN B, ACUTE kidney failure, RANDOM forest algorithms, ELECTRONIC health records

Abstract

Background: Liposomal amphotericin B (L-AmB) has become the mainstay of treatment for severe invasive fungal infections. However, the potential for renal toxicity must be considered. Aims: To evaluate the incidence of acute kidney injury (AKI) in critically ill patients receiving L-AmB for more than 48 h. Methods: Retrospective, observational, single-center study. Clinical, demographic and laboratory variables were obtained automatically from the electronic medical record. AKI incidence was analyzed in the entire population and in patients with a "low" or "high" risk of AKI based on their creatinine levels at the outset of the study. Factors associated with the development of AKI were studied using random forest models. Results: Finally, 67 patients with a median age of 61 (53–71) years, 67% male, a median SOFA of 4 (3–6.5) and a crude mortality of 34.3% were included. No variations in serum creatinine were observed during the observation period, except for a decrease in the high-risk subgroup. A total of 26.8% (total population), 25% (low risk) and 13% (high risk) of patients developed AKI. Norepinephrine, the SOFA score, furosemide (general model), potassium, C-reactive protein and procalcitonin (low-risk subgroup) were the variables identified by the random forest models as important contributing factors to the development of AKI other than L-AmB administration. Conclusions: The development of AKI is multifactorial and the administration of L-AmB appears to be safe in this group of patients. [ABSTRACT FROM AUTHOR]

Published

2024

2. Predictive Factors of Piperacillin Exposure and the Impact on Target Attainment after Continuous Infusion Administration to Critically Ill Patients.

Author

Martínez-Casanova, Javier, Esteve-Pitarch, Erika, Colom-Codina, Helena, Gumucio-Sanguino, Víctor Daniel, Cobo-Sacristán, Sara, Shaw, Evelyn, Maisterra-Santos, Kristel, Sabater-Riera, Joan, Pérez-Fernandez, Xosé L., Rigo-Bonnin, Raül, Tubau-Quintano, Fe, Carratalà, Jordi, and Padullés-Zamora, Ariadna

Subjects

CRITICALLY ill, PIPERACILLIN, DRUG monitoring, BETA lactam antibiotics

Abstract

Critically ill patients undergo significant pathophysiological changes that affect antibiotic pharmacokinetics. Piperacillin/tazobactam administered by continuous infusion (CI) improves pharmacokinetic/pharmacodynamic (PK/PD) target attainment. This study aimed to characterize piperacillin PK after CI administration of piperacillin/tazobactam in critically ill adult patients with preserved renal function and to determine the empirical optimal dosing regimen. A total of 218 piperacillin concentrations from 106 patients were simultaneously analyzed through the population PK approach. A two-compartment linear model best described the data. Creatinine clearance (CLCR) estimated by CKD-EPI was the covariate, the most predictive factor of piperacillin clearance (CL) interindividual variability. The mean (relative standard error) parameter estimates for the final model were: CL: 12.0 L/h (6.03%); central and peripheral compartment distribution volumes: 20.7 L (8.94%) and 62.4 L (50.80%), respectively; intercompartmental clearance: 4.8 L/h (26.4%). For the PK/PD target of 100% fT>1×MIC, 12 g of piperacillin provide a probability of target attainment > 90% for MIC < 16 mg/L, regardless of CLCR, but higher doses are needed for MIC = 16 mg/L when CLCR > 100 mL/min. For 100% fT>4×MIC, the highest dose (24 g/24 h) was not sufficient to ensure adequate exposure, except for MICs of 1 and 4 mg/L. Our model can be used as a support tool for initial dose guidance and during therapeutic drug monitoring. [ABSTRACT FROM AUTHOR]

Published

2023