A. Banting scite author profile

A. Banting

5Publications

92Citation Statements Received

26Citation Statements Given

How they've been cited

104

How they cite others

Affiliations

École Nationale Vétérinaire d'Alfort

Publications

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Efficacy of oral and parenteral ketoprofen in lactating cows with endotoxin‐induced acute mastitis

Banting¹,

Banting²,

Heinonen

et al. 2008

Veterinary Record

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One hind quarter of 27 healthy lactating cows was infused with 100 microg Escherichia coli endotoxin. Two hours later, nine of the cows were given physiological saline by intramuscular injection, nine were given 4 mg/kg ketoprofen orally, and nine were given 3 mg/kg ketoprofen by intramuscular injection. Ketoprofen administered either orally or parenterally significantly reduced the effect of the endotoxin on rectal temperature, ruminal contractions and respiratory rate. The size of the udder, the signs of pain and the concentrations of thromboxane B2, especially in plasma, were also reduced, and the appearance of their milk was almost normal. The response of cows to the oral treatment was as rapid as it was to intramuscular treatment.

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Comparison of the pharmacokinetics and local tolerance of three injectable oxytetracycline formulations in pigs

Banting¹,

Baggot²

1996

Vet Pharm & Therapeutics

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The pharmacokinetic properties and local tolerance of three oxytetracycline formulations, one conventional (Engemycine, 10%) and two long-acting (Oxyter LA, 20% and Terramycin LA, 20%) were compared in clinically healthy cross-bred pigs following intramuscular injection of single doses (20 mg/kg body weight) in the neck region. Non-compartmental methods were used to calculate the pharmacokinetic parameters. Assessment of local tolerance was based on serum creatine phosphokinase (CPK) concentration and a combination of echographical, macroscopic and histological examinations of the intramuscular injection site. Statistically significant differences (one-way analysis of variance, F-test) were obtained between the three formulations in peak plasma concentration, peak time and mean residence time. Area under the curve did not differ significantly between the formulations. Using the Students t-test for paired data, the two long-acting formulations differed significantly in peak plasma concentration and peak time. Both of the long-acting formulations differed significantly from the conventional formulation in the peak time and mean residence time. All three formulations produced an increase in serum CPK concentrations. The increase in CPK concentration was present from 6 to 24 h post treatment for Terramycin LA, from 6 to 72 h for Oxyter LA and from 6 to 96 h for Engemycine (the conventional formulation). Echographical examination of the injection site showed lesions of an inflammatory type up to 96 h after IM injection of the drug products, whereas from 7 days the lesions represented primarily scar formation. Histological examination of tissue from the injection site did not correlate with echographical scores. The results obtained in this study show that the long-acting formulations provide significantly longer mean residence times of oxytetracycline than the conventional formulation, and that local tolerance at the IM injection site was similar for all three formulations under the experimental conditions used in this study. It can be concluded that the long-acting formulations provide the advantage of a longer dosage interval when administered to pigs by intramuscular injection in the neck region at a dose of 20 mg/kg body weight.

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Review of disorders of the ruminant digit with proposals for anatomical and pathological terminology and recording

Weaver¹,

Andersson²,

Banting³

et al. 1981

Veterinary Record

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Dose‐response investigation of oral ketoprofen in pigs challenged with Escherichia coli endotoxin

Mustonen

Banting²,

Raekallio

et al. 2012

Veterinary Record

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In order to determine the effective dose, the effects of orally administered ketoprofen were evaluated in pigs following intravenous challenge with Escherichia coli endotoxin. One hour after the challenge, five groups of pigs were treated with either tap water or ketoprofen (0.5 mg/kg, 1 mg/kg, 2 mg/kg or 4 mg/kg). The body temperature was measured and a total clinical score was calculated after assessing the general behaviour, respiratory rate and locomotion of the pigs. Thromboxane B(2) and ketoprofen concentrations were analysed from blood samples. Ketoprofen treatment significantly reduced the rectal temperature and total clinical scores, and lowered blood thromboxane B(2) concentrations when compared with the control group. Ketoprofen plasma concentrations were lower than previously reported in healthy pigs after similar doses. The appropriate dose of orally administered ketoprofen in pigs in this model is 2 mg/kg, as the higher dose of 4 mg/kg failed to provide an additional benefit.

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Pathophysiological Studies of Experimental Fasciola Hepatica Infections in Sheep and Rabbits

Bars

Banting

1976

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A. Banting

Efficacy of oral and parenteral ketoprofen in lactating cows with endotoxin‐induced acute mastitis

Comparison of the pharmacokinetics and local tolerance of three injectable oxytetracycline formulations in pigs

Review of disorders of the ruminant digit with proposals for anatomical and pathological terminology and recording

Dose‐response investigation of oral ketoprofen in pigs challenged with Escherichia coli endotoxin

Pathophysiological Studies of Experimental Fasciola Hepatica Infections in Sheep and Rabbits

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