Population Pharmacokinetics of Cis-, Trans-, and Total Cefprozil in Healthy Male Koreans

Jang, Ji-Hun; Jeong, Seung‐Hyun; Cho, Hea-Young; Lee, Yong-Bok

doi:10.3390/pharmaceutics11100531

Cited by 10 publications

(7 citation statements)

References 29 publications

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“…This was related to the report that the activity of cytochrome P450 and phase II conjugation related to drug metabolism is increased with weight gain [27]. In addition, correlations between potential covariates and parameters used in the cefaclor population pharmacokinetic model shown in Figure 2 have also been reported in studies on pharmacokinetic analysis and modeling of other drugs [13,14]. Figure S1 shows graph results of those whose degrees of correlation were confirmed after those shown in Figure 2.…”

Section: Population Pharmacokinetic Model Analysissupporting

confidence: 64%

“…According to a previous report, cefaclor and cefprozil were mostly excreted in the urine through the kidney [20]. A correlation between CrCl and CL/F was confirmed in a population pharmacokinetic model of cefprozil for healthy adults, and that correlation was considered the main covariate [13]. For cefaclor, the correlation between CrCl and CL/F was reflected as the main covariate, similar to that found for cefprozil.…”

Section: Population Pharmacokinetic Model Analysissupporting

confidence: 64%

“…Construction and analysis of cefaclor's population pharmacokinetic model was performed using a non-linear mixed effects model with Phoenix nonlinear mixed effects model (NLME) software version 8.3 (Pharsight, Certara Inc.). Population pharmacokinetic analysis of drugs using this program has been actively performed [13,14]. Population pharmacokinetic model development for cefaclor was performed in the first-order conditional estimates method with extended least squares estimation (with N-ε interaction).…”

Section: Model Developmentmentioning

confidence: 99%

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Population Pharmacokinetic Analysis of Cefaclor in Healthy Korean Subjects

et al. 2021

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The aims of this study were: (1) to perform population pharmacokinetic analysis of cefaclor in healthy Korean subjects, and (2) to investigate possible effects of various covariates on pharmacokinetic parameters of cefaclor. Although cefaclor belongs to the cephalosporin family antibiotic that has been used in various indications, there have been very few population studies on factors affecting its pharmacokinetics. Therefore, this study is very important in that effective therapy could be possible through a population pharmacokinetic study that explores effective covariates related to cefaclor pharmacokinetic diversity between individuals. Pharmacokinetic results of 48 subjects with physical and biochemical parameters were used for the population pharmacokinetic analysis of cefaclor. A one-compartment with lag-time and first-order absorption/elimination was constructed as a base model and extended to include covariates that could influence between-subject variability. Creatinine clearance and body weight significantly influenced systemic clearance and distribution volume of cefaclor. Cefaclor’s final population pharmacokinetic model was validated and some of the population’s pharmacokinetic diversity could be explained. Herein, we first describe the establishment of a population pharmacokinetic model of cefaclor for healthy Koreans that might be useful for customizing cefaclor or exploring additional covariates in patients.

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Section: Population Pharmacokinetic Model Analysissupporting

confidence: 64%

Section: Population Pharmacokinetic Model Analysissupporting

confidence: 64%

Section: Model Developmentmentioning

confidence: 99%

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Population Pharmacokinetic Analysis of Cefaclor in Healthy Korean Subjects

et al. 2021

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“…Construction and analysis of the population pharmacokinetic model of methotrexate-loaded nanoparticles and nanoemulsions (and free methotrexate solution) were performed using a nonlinear mixed effects (NLME) model approach using Phoenix NLME (version 8.3, Pharsight, Certara Inc., Princeton, NJ, USA) software. This is a popular choice for population pharmacokinetic analysis of drugs [ 18 , 19 ]. Population pharmacokinetic model development was performed using the first-order conditional estimates method with extended least squares estimation (with ŋ – ε interaction).…”

Section: Methodsmentioning

confidence: 99%

Pharmacokinetic Comparison between Methotrexate-Loaded Nanoparticles and Nanoemulsions as Hard- and Soft-Type Nanoformulations: A Population Pharmacokinetic Modeling Approach

2021

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The purpose of this study was to identify and explore the differences in pharmacokinetics between different nanoformulations. This was done by comparing the pharmacokinetics of methotrexate-loaded nanoparticles [poly(lactic-co-glycolic acid); size of 163.70 ± 10.25 nm] and nanoemulsions (olive oil and Labrasol; size of 173.77 ± 5.76 nm), which represent hard- and soft-type nanoformulations, respectively. In addition, the population pharmacokinetic modeling approach as a useful tool for the comparison of pharmacokinetics between nanoformulations was newly proposed through this study. Significant pharmacokinetic differences were identified between nanoformulations through the new population pharmacokinetic modeling approach. As a result, the formulation type was explored as a significant covariate. The clearance and bioavailability of methotrexate-loaded nanoemulsions tended to decrease by 99% and increase by 19%, respectively, compared to those of the nanoparticles. The exploration of significant pharmacokinetic differences between drug formulations and their correlations presented in this study provide new perspectives on the development of nanoformulations.

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“…Population pharmacokinetic variability and modeling studies of drugs are very useful scientific approaches to finding effective dosage regimens based on quantitative predictions [ [11] , [12] , [13] ]. Consideration of efficacy and safety through identification of the pharmacokinetic diversity of fexofenadine among individuals will be a very important concern in clinical practice [ [14] , [15] , [16] ]. Depending on the continuous exposure of fexofenadine, the pharmacokinetic variability among individuals may obviously appear, and this may lead to failure to reach the appropriate therapeutic target range or side effects (common reported side effects of fexofenadine: headaches, feeling sleepy, dry mouth, feeling sick, and dizziness) due to excessive accumulation.…”

Section: Introductionmentioning

confidence: 99%