Estimation of residue depletion of cyadox and its marker residue in edible tissues of pigs using physiologically based pharmacokinetic modelling

Huang, Lingli; Lin, Zhoumeng; Zhou, Xuan; Zhu, Meiling; Gehring, Ronette; Riviere, Jim E.; Zhang, Yuan

doi:10.1080/19440049.2015.1100330

Cited by 16 publications

(35 citation statements)

References 45 publications

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“…This modeling strategy represents a significant advance in this field because published PBPK models for veterinary drugs all focus on a single drug or one species181920212223. These available models have different model structures that prevent direct comparisons of the pharmacokinetics of different drugs across species.…”

Section: Discussionmentioning

confidence: 99%

“…Physiological parameters for cattle and swine were obtained from the literature182022 and are provided in Supplementary Table 2. Initial values for partition coefficients were obtained from earlier PBPK models for flunixin and sulfamethazine2022, or calculated using tissue:plasma AUC (area under the concentration curve) ratio method based on pharmacokinetic data in cattle for enrofloxacin29, or based on the reported tissue penetration factors for ceftiofur27.…”

Section: Methodsmentioning

confidence: 99%

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Human Food Safety Implications of Variation in Food Animal Drug Metabolism

Lin

Vahl

Riviere

2016

Sci Rep

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Violative drug residues in animal-derived foods are a global food safety concern. The use of a fixed main metabolite to parent drug (M/D) ratio determined in healthy animals to establish drug tolerances and withdrawal times in diseased animals results in frequent residue violations in food-producing animals. We created a general physiologically based pharmacokinetic model for representative drugs (ceftiofur, enrofloxacin, flunixin, and sulfamethazine) in cattle and swine based on extensive published literature. Simulation results showed that the M/D ratio was not a fixed value, but a time-dependent range. Disease changed M/D ratios substantially and extended withdrawal times; these effects exhibited drug- and species-specificity. These results challenge the interpretation of violative residues based on the use of the M/D ratio to establish tolerances for metabolized drugs.

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Human Food Safety Implications of Variation in Food Animal Drug Metabolism

Lin

Vahl

Riviere

2016

Sci Rep

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“…In recent years, there has been an increase in the applications of physiologically based pharmacokinetic (PBPK) models to predict veterinary drug residues (Huang et al., ; Li, Gehring, Riviere, & Lin, ; Yang, Huang, et al., ; Yang et al., ; Yang, Sun, Liu, & Zeng, ; Yang, Sun, et al., ; Yang et al., ; Zeng et al., ). Compared with the traditional monitoring method after animal slaughter, the PBPK model is based on mass‐balance equations defined by physiological mechanisms, and it is predictive in nature and allows for the use of in vitro mechanistic data and population variability data to predict the distribution of drug in animals (Lin, Gehring, Mochel, Lave, & Riviere, ).…”

Section: Introductionmentioning

confidence: 99%

Development of a multiroute physiologically based pharmacokinetic model for orbifloxacin in rabbits

Yang

Shi

et al. 2018

Vet Pharm & Therapeutics

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To predict the orbifloxacin concentrations in rabbits after multiple routes of administration, a flow-limited multiroute physiologically based pharmacokinetic (PBPK) model was developed. Three routes of administration (IV, IM, and PO) were incorporated into this model. Physiological parameters including tissue weights and blood flows through different tissues were obtained from the literature. The tissue/plasma partition coefficients (P s) for noneliminating tissues were calculated according to the area method, while the P s for kidney and the rest of the body compartment, together with other parameters for absorption and elimination, were optimized based on the published concentrations. The comparisons between predicted and observed orbifloxacin concentrations proved its validity, and the present model predicted available concentration data well, including those in liver, kidney, muscle, lung, heart, and plasma after oral, intravenous, or intramuscular administration. A local sensitivity analysis was also performed, which showed that the parameters for oral absorption were most influential on the orbifloxacin concentrations. This model was used to predict plasma and tissue concentrations after multiple oral or intramuscular administration. This study demonstrated the feasibility of predicting drug residues in minor species after multiple routes of administration in the extra-label manner using the PBPK modeling.

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“…In the last decade, PBPK modeling has been widely used in the area of veterinary medicine, from the prediction of drug tissue residues (Huang et al, ; Leavens et al, ; Yang et al, ), estimating the withdrawal time (Buur, Baynes, Smith, & Riviere, ; Yang, Huang, et al, ; Yang, Zhou, et al, ), to facilitating the food safety assessment (Henri, Carrez, Meda, Laurentie, & Sanders, ; Lin, Gehring, Mochel, Lavé, & Riviere, ; Yang, Huang, et al, ; Yang, Zhou, et al, ). In this study, a PBPK model was established for heavy sows based on a previous generic PBPK model for swine and cattle (Li et al, ).…”

Section: Discussionmentioning

confidence: 99%

An integrated experimental and physiologically based pharmacokinetic modeling study of penicillin G in heavy sows

Mainquist-Whigham

Karriker

et al. 2019

Vet Pharm & Therapeutics

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Penicillin G is widely used in food‐producing animals at extralabel doses and is one of the most frequently identified violative drug residues in animal‐derived food products. In this study, the plasma pharmacokinetics and tissue residue depletion of penicillin G in heavy sows after repeated intramuscular administrations at label (6.5 mg/kg) and 5 × label (32.5 mg/kg) doses were determined. Plasma, urine, and environmental samples were tested as potential antemortem markers for penicillin G residues. The collected new data and other available data from the literature were used to develop a population physiologically based pharmacokinetic (PBPK) model for penicillin G in heavy sows. The results showed that antemortem testing of urine provided potential correlation with tissue residue levels. Based on the United States Department of Agriculture Food Safety and Inspection Service action limit of 25 ng/g, the model estimated a withdrawal interval of 38 days for penicillin G in heavy sows after 3 repeated intramuscular injections at 5 × label dose. This study improves our understanding of penicillin G pharmacokinetics and tissue residue depletion in heavy sows and provides a tool to predict proper withdrawal intervals after extralabel use of penicillin G in heavy sows, thereby helping safety assessment of sow‐derived meat products.

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Estimation of residue depletion of cyadox and its marker residue in edible tissues of pigs using physiologically based pharmacokinetic modelling

Cited by 16 publications

References 45 publications

Human Food Safety Implications of Variation in Food Animal Drug Metabolism

Human Food Safety Implications of Variation in Food Animal Drug Metabolism

Development of a multiroute physiologically based pharmacokinetic model for orbifloxacin in rabbits

An integrated experimental and physiologically based pharmacokinetic modeling study of penicillin G in heavy sows

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