Pharmacokinetics and relative bioavailability of an oral amoxicillin-apramycin combination in pigs

Dai, Chongshan; Zhao, Tingting; Yang, Xing; Xiao, Xia; Velkov, Tony; Tang, Shusheng

doi:10.1371/journal.pone.0176149

Cited by 7 publications

(6 citation statements)

References 24 publications

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“…PK studies on APR were mainly based on PK data in plasma. Previous result showed that the peak plasma concentration of APR was 0.23 µg/mL and reached at 2.25 h, the AUC INF was 1.59 h•µg/mL in plasma after oral administration of 4 mg/kg [24]. The corresponding PK parameters of the C max and AUC INF were lower observed in plasma of pigs and in broiler chickens [25,26].…”

Section: Discussionmentioning

confidence: 91%

Clinical Breakpoint of Apramycin to Swine Salmonella and Its Effect on Ileum Flora

Dai

Guo

et al. 2022

IJMS

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The purpose of this study was to establish the clinical breakpoint (CBP) of apramycin (APR) against Salmonella in swine and evaluate its effect on intestinal microbiota. The CBP was established based on three cutoff values of wild-type cutoff value (COWT), pharmacokinetic-pharmadynamic (PK/PD) cutoff value (COPD) and clinical cutoff value (COCL). The effect of the optimized dose regimen based on ex vivo PK/PD study. The evolution of the ileum flora was determined by the 16rRNA gene sequencing and bioinformatics. This study firstly established the COWT, COPD in ileum, and COCL of APR against swine Salmonella, the value of these cutoffs were 32 µg/mL, 32 µg/mL and 8 µg/mL, respectively. According to the guiding principle of the Clinical Laboratory Standards Institute (CLSI), the final CBP in ileum was 32 µg/mL. Our results revealed the main evolution route in the composition of ileum microbiota of diarrheic piglets treated by APR. The change of the abundances of Bacteroidetes and Euryarchaeota was the most obvious during the evolution process. Methanobrevibacter, Prevotella, S24-7 and Ruminococcaceae were obtained as the highest abundance genus. The abundance of Methanobrevibacter increased significantly when APR treatment carried and decreased in cure and withdrawal period groups. The abundance of Prevotella in the tested groups was significantly lower than that in the healthy group. A decreased of abundance in S24-7 was observed after Salmonella infection and increased slightly after cure. Ruminococcaceae increased significantly after Salmonella infection and decreased significantly after APR treatment. In addition, the genera of Methanobrevibacter and Prevotella were defined as the key node. Valine, leucine and isoleucine biosynthesis, D-Glutamine and D-glutamate metabolism, D-Alanine metabolism, Peptidoglycan and amino acids biosynthesis were the top five Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways in the ileum microbiota of piglets during the Salmonella infection and APR treatment process. Our study extended the understanding of dynamic shift of gut microbes during diarrheic piglets treated by APR.

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Section: Discussionmentioning

confidence: 91%

Clinical Breakpoint of Apramycin to Swine Salmonella and Its Effect on Ileum Flora

Dai

Guo

et al. 2022

IJMS

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“…It was not possible to study the consumption of the medicated feed by the (individual) pigs in the current study. However, other studies [9,10,15] show a large variability in feed consumption between pigs housed in the same pen and stable. Given this large variability, the risk is estimated to be 'moderate to high' based on available literature.…”

Section: • Module 4: Consumption Of Medicated Feed By the Pigsmentioning

confidence: 95%

“…For antimicrobial treatment to be efficacious, several parameters play a crucial role: the choice of the medicine, the homogeneity and stability of the drug in feed or water [6,7], the dose ingested by the individual animal, and drug factors that affect whether or not the pharmacokinetic/pharmacodynamic (PK/PD) breakpoint is reached [8]. Noticeably, high variability in plasma concentrations is observed in individual pigs after the provision of medicated feed [9,10] and drinking water [11][12][13][14]. Several reasons can account for this variability, namely different intake due to social hierarchy and (sub)clinical illness, homogeneity, stability as well as palatability [2,[15][16][17].…”

Section: Introductionmentioning

confidence: 99%

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Qualitative risk assessment of homogeneity, stability, and residual concentrations of antimicrobials in medicated feed and drinking water in pig rearing

et al. 2023

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Background Despite the common use of oral group treatment in pig rearing, the magnitude of the factors influencing the homogeneity and stability of antimicrobial drugs in medicated feed and medicated drinking water are largely unknown, as well as the residual concentrations of the drugs after the end of the treatment. Results This study presents a qualitative risk assessment to estimate the magnitude of the risks for reduced homogeneity and stability, and increased residual concentrations of antimicrobial drugs in medicated feed and drinking water on the farm. Risk assessment was done using a questionnaire and farm visits (n = 52), combined with a second questionnaire, and concentrations of amoxicillin and doxycycline measured in medicated feed and water samples, each collected on 10 farms. For medicated feed, the duration of storage in the silo did not show to influence the concentration levels in a consistent trend, while the treatment duration had a low to negligible effect. A moderate to high risk was found caused by human error when preparing the medicated feed on the farm. Purchased medicated feed greatly reduces the risk of human error and drugs remain stable during the duration of treatment, while the risk of residual concentrations after the end of the treatment was estimated to be low to moderate. The feed intake variability was identified as a moderate to high risk factor. For medicated drinking water, the type of dosing pump, age of pre-solution, and human errors during the preparation of the pre-solution present a moderate to high risk on homogeneity and stability. Precipitation of the active substance in the absence of a stirrer in a drinking water tank was shown to be a low to moderate risk factor for residues after treatment. Waterline length had a weak correlation with the concentrations of the antimicrobials, while a moderate to high influence was detected for the water intake by the pigs. Conclusions A considerable variation in drug concentration in both medicated feed and medicated drinking water was detected depending on their preparation. Therefore, it is important to know which factors influence the homogeneity and stability, and the residual concentrations after treatment.

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“…The bioavailability of apramycin is very low; about 4% in pigs (Dai et al., 2017 ) and 2% in broilers (Afifi and Ramadan, 1997 ). Very low serum concentrations were also described after oral administration to calves (Ziv et al., 1985 ).…”

Section: Introductionmentioning

confidence: 99%

Maximum levels of cross‐contamination for 24 antimicrobial active substances in non‐target feed. Part 2: Aminoglycosides/aminocyclitols: apramycin, paromomycin, neomycin and spectinomycin

Koutsoumanis¹,

Allende²,

Álvarez‐Ordóñez³

et al. 2021

EFS2

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The specific concentrations of apramycin, paromomycin, neomycin and spectinomycin in non-target feed for food-producing animals, below which there would not be an effect on the emergence of, and/or selection for, resistance in bacteria relevant for human and animal health, as well as the specific antimicrobial concentrations in feed which have an effect in terms of growth promotion/increased yield, were assessed by EFSA in collaboration with EMA. Details of the methodology used for this assessment, associated data gaps and uncertainties, are presented in a separate document. To address antimicrobial resistance, the Feed Antimicrobial Resistance Selection Concentration (FARSC) model developed specifically for the assessment was applied. However, due to the lack of data on the parameters required to calculate the FARSC for these antimicrobials, it was not possible to conclude the assessment until further experimental data become available. To address growth promotion, data from scientific publications obtained from an extensive literature review were used. Levels in feed that showed to have an effect on growth promotion/increased yield were reported for apramycin and neomycin, whilst for paromomycin and spectinomycin, no suitable data for the assessment were available. It was recommended to carry out studies to generate the data that are required to fill the gaps which prevented the calculation of the FARSC for these four antimicrobials.

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Pharmacokinetics and relative bioavailability of an oral amoxicillin-apramycin combination in pigs

Cited by 7 publications

References 24 publications

Clinical Breakpoint of Apramycin to Swine Salmonella and Its Effect on Ileum Flora

Clinical Breakpoint of Apramycin to Swine Salmonella and Its Effect on Ileum Flora

Qualitative risk assessment of homogeneity, stability, and residual concentrations of antimicrobials in medicated feed and drinking water in pig rearing

Maximum levels of cross‐contamination for 24 antimicrobial active substances in non‐target feed. Part 2: Aminoglycosides/aminocyclitols: apramycin, paromomycin, neomycin and spectinomycin

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Pharmacokinetics and relative bioavailability of an oral amoxicillin-apramycin combination in pigs

Cited by 7 publications

References 24 publications

Clinical Breakpoint of Apramycin to Swine Salmonella and Its Effect on Ileum Flora

Clinical Breakpoint of Apramycin to Swine Salmonella and Its Effect on Ileum Flora

Qualitative risk assessment of homogeneity, stability, and residual concentrations of antimicrobials in medicated feed and drinking water in pig rearing

Maximum levels of cross‐contamination for 24 antimicrobial active substances in non‐target feed. Part 2: Aminoglycosides/aminocyclitols: apramycin, paromomycin, neomycin and spectinomycin

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Product

Resources

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Maximum levels of cross‐contamination for 24 antimicrobial active substances in non‐target feed. Part 2: Aminoglycosides/aminocyclitols: apramycin, paromomycin, neomycin and spectinomycin