S. Burgaud scite author profile

S. Burgaud

5Publications

75Citation Statements Received

101Citation Statements Given

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Département Santé Animale

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Pharmacokinetics of total thyroxine in dogs after administration of an oral solution of levothyroxine sodium

Traon¹,

Burgaud²,

Horspool³

2008

Vet Pharm & Therapeutics

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Oral L-thyroxine (L-T4) supplementation is used to replace thyroid hormone concentrations in dogs with hypothyroidism. The pharmacokinetics of L-T4 following administration of a solution (Leventa) was investigated in healthy dogs. L-T4 was absorbed fairly rapidly (t(max) 3 h). A mean bioavailability of 22% was calculated following a single oral administration of 40 microg L-T4/kg body weight. Repeated oral administration at the same dose for 14 consecutive days did not lead to any accumulation of T4 in serum. After intravenous administration of L-T4, a serum half-life of 11.6 h was calculated. Food intake concomitant with L-T4 oral administration delayed L-T4 absorption and decreased its rate and extent by about 45%. The relative bioavailability of L-T4 following administration of a tablet formulation was about 50% of that of the L-T4 solution. The pharmacokinetic properties of liquid L-T4 after oral administration support the use of a dose rate of 20 microg/kg once daily, as a starting dose for replacement therapy in dogs with hypothyroidism.

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Clinical efficacy and safety of a once‐daily formulation of carbimazole in cats with hyperthyroidism

Frénais

Rosenberg

Burgaud

et al. 2009

J of Small Animal Practice

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Pharmacokinetics of controlled‐release carbimazole tablets support once daily dosing in cats

Frénais¹,

Burgaud²,

Horspool

2008

Vet Pharm & Therapeutics

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Carbimazole, a prodrug of methimazole, is used in the treatment of hyperthyroidism in cats. The pharmacokinetics of methimazole was investigated in healthy cats following oral administration of 15 mg of carbimazole as a controlled-release tablet (Vidalta), Intervet). The controlled-release tablet did not produce a pronounced concentration peak and methimazole was present in the circulation for a sustained period, compared with a conventional tablet formulation. The time to reach peak concentrations after carbimazole administration was quite long (t(max) 6 h). The absolute bioavailability of carbimazole was around 88 +/- 11%. Repeated oral administration daily for 13 consecutive days did not lead to accumulation of methimazole in plasma. The extent of absorption of carbimazole was about 40% higher when administered to cats that had been fed compared to fasted cats. The relative oral bioavailability of methimazole following administration of the controlled-release tablets was similar to that of a conventional release formulation (83 +/- 21%). The pharmacokinetics of this controlled-release formulation of carbimazole supports its use as a once daily treatment (both as a starting dose and for maintenance therapy) for cats with hyperthyroidism.

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Clinical Evaluation of a Novel Liquid Formulation of L‐Thyroxine for Once Daily Treatment of Dogs with Hypothyroidism

Traon

Brennan

Burgaud

et al. 2009

Veterinary Internal Medicne

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Background: A liquid solution of levothyroxine (L-T4) is available for treatment of canine hypothyroidism. Hypothesis: Once daily oral administration of a liquid L-T4 solution is effective and safe for controlling hypothyroidism in dogs.Animals: Thirty-five dogs with naturally occurring hypothyroidism. Methods: Dogs received L-T4 solution PO once daily at a starting dosage of 20 mg/kg body weight (BW). The dose was adjusted every 4 weeks, based on clinical signs and peak serum total T4 (tT4) concentrations. Target peak serum tT4 and thyroid stimulating hormone (TSH) concentrations, 4-6 hours posttreatment, were 35-95 nmol/L and o 0.68 ng/mL, respectively. Dogs were followed for up to 22 weeks after establishment of the maintenance dose.Results: Clinical signs of hypothyroidism improved or resolved in 91% of dogs after 4 weeks of L-T4 treatment at 20 mg/kg once daily. The maintenance dose was established in 76, 94, and 100% of dogs after 4, 8, and 12 weeks of treatment, respectively. This was 20 mg L-T4/kg BW for 79% of the dogs, 30 mg/kg BW for 15%, and 10-15 mg/kg BW in the remaining 6%, once daily. Thereafter, median peak tT4 and TSH concentrations were 51 nmol/L and 0.18 ng/mL, respectively, and remained stable during the 22-week follow-up; clinical signs did not recur.Conclusions and Clinical Importance: All of the hypothyroid dogs had rapid clinical and hormonal responses to supplementation with the PO-administered L-T4 solution. The starting dosage of 20 mg L-T4/kg BW once daily was suitable for 79% of dogs.

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Pharmacokinetics and pharmacodynamics of ramipril and ramiprilat in healthy cats

Desmoulins¹,

Burgaud²,

Horspool

2008

Vet Pharm & Therapeutics

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The pharmacokinetics of ramipril and its active metabolite, ramiprilat, was determined in cats following single and repeated oral doses of ramipril (Vasotop tablets) (once daily for 9 days) at dose rates of 0.125, 0.25, 0.5 and 1.0 mg/kg. The pharmacodynamic effects were assessed by measuring plasma angiotensin-converting enzyme (ACE) activity. Maximum ramipril concentrations were attained within 30 min following a single dose and declined rapidly (concentrations were below the limit of quantification 4 h after treatment). Peak ramiprilat concentrations were detected at approximately 1.5 h. The apparent terminal half-life (t((1/2)beta)) was > or =20 h irrespective of the dose. Ramiprilat accumulated in plasma (ratio of accumulation 1.3 to 1.9 depending on the dose rate) following repeated administration. Steady-state conditions were attained after the second dose. Excretion was predominant in faeces (87%) and to a lesser extent in urine (11%). The rate and extent of absorption of ramipril as well as its conversion to ramiprilat were not significantly influenced by the presence of food in the gastrointestinal tract. Plasma-ACE activity was almost completely abolished 0.5-2.0 h after treatment, irrespective of the dose rate. Significant inhibition of ACE activity of 54.7 to 82.6% (depending on the dosage) was still present 24 h after treatment. Treatment was well-tolerated in all cats. Ramipril at a dose rate of 0.125 mg/kg once daily produces significant and long-lasting inhibition of ACE activity in healthy cats. The appropriateness of this dosage regime needs to be confirmed in diseased cats.

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S. Burgaud

Pharmacokinetics of total thyroxine in dogs after administration of an oral solution of levothyroxine sodium

Clinical efficacy and safety of a once‐daily formulation of carbimazole in cats with hyperthyroidism

Pharmacokinetics of controlled‐release carbimazole tablets support once daily dosing in cats

Clinical Evaluation of a Novel Liquid Formulation of L‐Thyroxine for Once Daily Treatment of Dogs with Hypothyroidism

Pharmacokinetics and pharmacodynamics of ramipril and ramiprilat in healthy cats

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