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6 results on '"Sulfanilamides blood"'

1. Determination of trimethoprim and sulphadoxine residues in porcine tissues and plasma.

Author

Boison JO, Nachilobe P, Cassidy R, Keng L, Thacker PA, Peacock A, Fesser AC, Lee S, Korsrud GO, and Bulmer WS

Subjects
Animals, Anti-Infective Agents, Urinary administration & dosage, Anti-Infective Agents, Urinary blood, Chromatography, High Pressure Liquid veterinary, Chromatography, Thin Layer veterinary, Female, Injections, Intramuscular, Sulfadoxine administration & dosage, Sulfadoxine blood, Sulfanilamides administration & dosage, Sulfanilamides blood, Trimethoprim administration & dosage, Trimethoprim blood, Anti-Infective Agents, Urinary analysis, Kidney chemistry, Liver chemistry, Lung chemistry, Muscle, Skeletal chemistry, Sulfadoxine analysis, Sulfanilamides analysis, Swine metabolism, Trimethoprim analysis
Abstract

Healthy gilts and market-ready hogs were administered a single intramuscular (IM) injection of Borgal, a commercial formulation of trimethoprim-sulfadoxine (TMP-SDX), once or twice daily. The objectives were to determine if a newly-developed high-performance liquid chromatographic (HPLC) method would be suitable for measuring the residual concentrations of TMP in the plasma of these live animals, and to determine if the administration of this veterinary drug would leave measurable residues in their plasma and tissues at slaughter. Plasma and tissue concentrations of SDX and TMP from these animals were determined over a period of 14 d using thin-layer chromatography/densitometry (TLCD), and the newly-developed HPLC method, respectively. The lowest detectable limit (LDL) for SDX in plasma and tissue was 20 ppb by TLCD. The HPLC method had a LDL of 5 ppb for TMP in plasma and tissue. Both methods were then used to provide baseline data on the absorption and depletion of TMP and SDX from these healthy animals. It was observed that both TMP and SDX were readily absorbed into the blood and tissues, but TMP was eliminated much faster than SDX. No TMP residues were detected in the plasma of any of the gilts at and beyond 21 h after drug administration. Also, no TMP residues were detected in the plasma of any of the market-ready hogs 24 h after drug administration at either the label dose or twice the label dose. Sulfadoxine residues at concentrations above the maximum residue limit (MRL) of 100 ppb were, however, detected in the plasma, muscle, kidney, liver, and injection sites of hogs slaughtered 1 and 3 d after a single IM administration at the label dose. Although SDX residues were still detectable in the lungs, kidney, liver and plasma of some hogs 10 d after administration of the label dose and twice the label dose, these were below the MRL. Postmortem examination revealed necrosis and inflammation at the injection sites, but no visible deposits of the injected drug.

Published
1996

2. Pharmacokinetics and renal clearance of sulphadimidine, sulphamerazine and sulphadiazine and their N4-acetyl and hydroxy metabolites in pigs.

Author

Nouws JF, Mevius D, Vree TB, and Degen M

Subjects
Animals, Male, Sulfadiazine blood, Sulfadiazine metabolism, Sulfadiazine pharmacokinetics, Sulfamerazine blood, Sulfamerazine metabolism, Sulfamerazine pharmacokinetics, Sulfamethazine analogs & derivatives, Sulfamethazine blood, Sulfamethazine metabolism, Sulfamethazine pharmacokinetics, Sulfanilamides blood, Sulfanilamides metabolism, Kidney metabolism, Sulfanilamides pharmacokinetics, Swine metabolism
Abstract

The effect of molecular structure on the drug disposition and protein binding in plasma, the urinary recovery, and the renal clearance of sulphamerazine (SMR), sulphadiazine (SDZ), and sulphadimidine (SDM) and their N4-acetyl and hydroxy derivatives were studied in pigs. Following IV administration of SDM, SMR and SDZ, their mean elimination half-lives were 12.4 h, 4.3 h and 4.9 h respectively. The plasma concentrations of parent sulphonamide were higher than those of the metabolites, and ran parallel. The acetylated derivatives were the main metabolites; traces of 6-hydroxymethylsulphamerazine and 4-hydroxysulphadiazine were detected in plasma. The urine recovery data showed that in pigs acetylation is the major elimination pathway of SDM, SMR and SDZ; hydroxylation became more important in case of SMR (6-hydroxymethyl and 4-hydroxy derivatives) and SDZ (4-hydroxy derivatives) than in SDM. In pigs methyl substitution of the pyrimidine side chain decreased the renal clearance of the parent drug and made the parent compound less accessible for hydroxylation. Acetylation and hydroxylation speeded up drug elimination, because their renal clearance values were higher than those of the parent drug.

Published
1989
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6. Mammary and renal excretion of sulphadoxine and trimethoprim in cows.

Author

Davitiyananda D and Rasmussen F

Subjects
Animals, Blood, Creatinine metabolism, Female, Hydrogen-Ion Concentration, Infusions, Parenteral, Protein Binding, Sulfanilamides administration & dosage, Sulfanilamides blood, Trimethoprim administration & dosage, Trimethoprim blood, Urine, Cattle metabolism, Kidney metabolism, Mammary Glands, Animal metabolism, Milk metabolism, Sulfanilamides metabolism, Trimethoprim metabolism
Published
1974

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