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Topic:Drug

The topic of drugs and horses encompasses the study of various pharmacological agents used in equine medicine for therapeutic purposes. This includes the administration of medications for pain management, disease treatment, and performance enhancement. The pharmacokinetics and pharmacodynamics of drugs in horses are key areas of research, as they determine the absorption, distribution, metabolism, and excretion of these substances. Additionally, the topic covers the detection and regulation of substances in competitive equestrian sports to ensure fair play and animal welfare. This page compiles peer-reviewed research studies and scholarly articles that explore the effects, safety, and regulatory aspects of drug use in equine health and performance.
Pharmacology of narcotic analgesics in the horse: quantitative detection of morphine in equine blood and urine and logit-Log transformations of this data.
American journal of veterinary research    September 1, 1981   Volume 42, Issue 9 1523-1530 
Combie J, Blake JW, Ramey BE, Tobin T.Morphine was detected in equine biological fluids by a combination of liquid-liquid extraction and column chromatography, followed by derivatization and gas-liquid chromatographic assay, using electron capture detector. Recovery of morphine from the equine biological samples was poor. However, despite an overall recovery of less than 20%, this method had a detection limit of 0.2 ng/ml. Addition of 5,000 U of bovine liver beta-glucuronidase/ml of urine enabled detection of the drug in urine for up to 144 hours after horses were given 0.1 mg of morphine/kg of body weight. Morphine was found for ...
Clinical trials of oxibendazole for control of equine internal parasites including benzimidazole-resistant small strongyles.
Modern veterinary practice    September 1, 1981   Volume 62, Issue 9 679-682 
Drudge JH, Lyons ET, Tolliver SC, Kubis JE.No abstract available
Pentobarbitone sodium as an anaesthetic in the horse.
The Veterinary record    August 8, 1981   Volume 109, Issue 6 125 doi: 10.1136/vr.109.6.125-a
O'Scanaill T.No abstract available
Pharmacokinetics of a single, orally administered dose of digoxin in horses.
American journal of veterinary research    August 1, 1981   Volume 42, Issue 8 1412-1414 
Pedersoli WM, Ravis WR, Belmonte AA, McCullers RM.Digoxin (elixir, 0.022 mg/kg) was administered via stomach tube to healthy horses of mixed breeding and sexes. Serum digoxin concentrations reached a peak (2.21 +/- 0.6 ng/ml) at approximately 1 hour after dosing and had a half-life of 28.8 +/- 10.7 hours. Digoxin kinetics followed a triexponential curve, indicating that at least a 2 compartmental model is required to characterize the serum concentration-time curve after this route of administration. It was calculated that to achieve average serum concentrations of 1.1 ng/ml, an oral dose of 17.4 microgram of digoxin elixir/kg/day and an IV do...
Analysis of phenylbutazone and its metabolites by high performance liquid chromatography.
Equine veterinary journal    July 1, 1981   Volume 13, Issue 3 201-203 doi: 10.1111/j.2042-3306.1981.tb03489.x
Taylor JB, Lees P, Gerring EL.No abstract available
Pharmacokinetics of phenylbutazone and its metabolites in the horse.
Equine veterinary journal    July 1, 1981   Volume 13, Issue 3 152-157 doi: 10.1111/j.2042-3306.1981.tb03472.x
Gerring EL, Lees P, Taylor JB.Phenylbutazone was given orally to 2 groups of horses and the plasma levels of the drug and its 2 principal metabolites oxyphenbutazone and gamma-hydroxyphenylbutazone measured by high performance liquid chromatography. Animals in Group 1 received single oral doses in a range from 1.1 to 13.2 mg/kg and were sampled over the succeeding 24 h. Considerable individual variation was observed both in timing and magnitude of the plasma drug responses between horses, but 24 h after dosing a clear dose response relation was recorded. Group 2 horses were given the recommended therapeutic dosage regimen ...
Science and the administration of phenylbutazone.
Equine veterinary journal    July 1, 1981   Volume 13, Issue 3 144-145 doi: 10.1111/j.2042-3306.1981.tb03469.x
No abstract available
Laryngeal paralysis in Arabian foals associated with oral haloxon administration.
Equine veterinary journal    July 1, 1981   Volume 13, Issue 3 171-176 doi: 10.1111/j.2042-3306.1981.tb03477.x
Rose RJ, Hartley WJ, Baker W.Bilateral laryngeal paralysis is described in 5 Arabian and part-Arabian foals aged between 23 and 35 days. Tracheotomies resulted in complete relief of dyspnoea. Two cases showed recovery of abductor function of the right arytenoid cartilage after 3 weeks and one of these cases later recovered left abductor function. Four of the foals were autopsied at various times from one week to 6 months after the onset of respiratory obstruction. Histology of the recurrent laryngeal nerves showed active Wallerian degeneration and loss of nerve fibres in many fascicles in cases affected for one to 2 weeks...
Clinical trial of xylazine with ketamine in equine anaesthesia.
The Veterinary record    June 6, 1981   Volume 108, Issue 23 489-493 doi: 10.1136/vr.108.23.489
Hall LW, Taylor PM.One hundred anaesthetics were administered in a clinical trial to 95 equine patients, ranging in age from nine months to 19 years and in weight from 140 to 1270 kg, undergoing a variety of surgical procedures. Acepromazine maleate premedication (0.01 to 0.03 mg per kg intramuscularly) was given to seven animals, the remainder were not premedicated. Xylazine (1.1 mg per kg) was injected intravenously over a two minute period and after a pause of two minutes ketamine (2.2 mg per kg) was injected rapidly by the same route. For 30 procedures no other anaesthetic was given but in 59 cases anaesthes...
[Kinetics of anti-inflammatory drugs in serum and synovia of horses (author’s transl)].
DTW. Deutsche tierarztliche Wochenschrift    June 5, 1981   Volume 88, Issue 6 218-220 
Lehmann W, Wintzer HJ, Frey HH.No abstract available
Haloxon: critical tests of antiparasitic activity in equids.
American journal of veterinary research    June 1, 1981   Volume 42, Issue 6 1043-1045 
Lyons ET, Drudge JH, Tolliver SC.Critical tests were conducted in 14 naturally infected equids (13 horses and 1 pony) to evaluate the antiparasitic activity of haloxon. Single doses were administered by stomach tube to 3 horses and 1 pony (60 mg/kg of body weight), by addition to the feed of 3 horses (60 mg/kg), and intraorally by powder gun to 7 horses (65 mg/kg). Haloxon was efficacious (99% to 100%) against infections of Parascaris equorum, Oxyuris equi (mature and immature), and Strongylus vulgaris at both dosage levels. Probstmayria vivipara parasites were removed in 1 horse treated at 60 mg/kg by stomach tube and S equi...
Pharmacokinetic analysis of intravenously and orally administered quinidine in horses.
American journal of veterinary research    June 1, 1981   Volume 42, Issue 6 938-942 
McGuirk SM, Muir WW, Sams RA.A pharmacokinetic study was made, using 7 healthy adult horses (weighing between 400 and 560 kg) given quinidine gluconate IV and quinidine sulfate orally. The apparent volume of distribution of quinidine base was 3.10 +/- 0.79 L/kg, total body clearance was 5.49 +/- 2.40 ml/minute/kg, and plasma half-life was 6.65 +/- 3.00 hours. The systemic availability of quinidine sulfate after oral administration of a 10 mg/kg dose was 48.5 +/- 20.4%. Oral administrations of quinidine sulfate in doses of 10 mg/kg and 10 g produced peak plasma concentrations of 0.79 microgram/ml at 146 minutes and 1.47 mi...
Tioxidazole: evaluation of antiparasitic activity of a micronized formulation in horses by the critical test method.
American journal of veterinary research    June 1, 1981   Volume 42, Issue 6 1048-1049 
Lyons ET, Drudge JH, Tolliver SC.Antiparasitic activity of a micronized formulation of the benzothiazole compound, tioxidazole, at the dose rate of 11 mg/kg, was evaluated by the critical test method. Drug was given by stomach to 3 horses and on feed to 3 horses. Excellent removal activity was found for Strongylus vulgaris (100%) in 5 naturally infected horses, S edentatus (91% to 100%) in 5 horses, small strongyles (88% to 99%) in 6 horses, immature Oxyuris equi (100%) in 5 horses, and Parascaris equorum (100%) in 5 horses (a 6th horse had 10 small specimens present at necropsy). There was no measurable activity against bots...
The pharmacokinetics of meclofenamic acid in the horse.
Journal of veterinary pharmacology and therapeutics    June 1, 1981   Volume 4, Issue 2 147-156 doi: 10.1111/j.1365-2885.1981.tb00724.x
Snow DH, Baxter P, Whiting B.The pharmacokinetics of meclofenamic acid were studied in Thoroughbred horses and in ponies. After intravenous (i.v.) administration of either 2 mg/kg or 4 mg/kg sodium meclofenamate the elimination half-life was of the order of 0.9 h while the volume of distribution was found to be 0.128 litre/kg. Elimination was in accordance with a one-compartment model. Following oral administration of either meclofenamic acid (4 mg/kg) or sodium meclofenamate (4 mg/kg) a much longer terminal half-life than that calculated for Kel from i.v. data was found. This anomaly indicated that the 'flip-flop' phenom...
Inhalation anesthesia: drugs and techniques.
The Veterinary clinics of North America. Large animal practice    May 1, 1981   Volume 3, Issue 1 59-71 doi: 10.1016/s0196-9846(17)30146-5
Kelly AB, Steffey EP.No abstract available
Drugs used to produce standing chemical restraint in horses.
The Veterinary clinics of North America. Large animal practice    May 1, 1981   Volume 3, Issue 1 17-44 doi: 10.1016/s0196-9846(17)30144-1
Muir WW.No abstract available
Intravenous anesthesia: drugs and techniques.
The Veterinary clinics of North America. Large animal practice    May 1, 1981   Volume 3, Issue 1 195-208 doi: 10.1016/s0196-9846(17)30152-0
Short CE.No abstract available
Pharmacokinetics and behavioral effects of methylphenidate in Thoroughbred horses.
American journal of veterinary research    May 1, 1981   Volume 42, Issue 5 722-726 
Shults T, Kownacki AA, Woods WE, Valentine R, Dougherty J, Tobin T.In horses given (rapid IV) methylphenidate (Ritalin, alpha-phenyl-2-piperidinacetic acid methyl ester; 0.70 mg/kg), plasma concentrations of the drug decreased rapidly at first, with an apparent alpha half-life of about 19 minutes, and then more slowly, with an apparent beta half-life of about 2.4 hours. These data were well fitted by a 2-compartment open model. In blood, about 40% of the methylphenidate present was in the plasma fraction, and of this, about 80% was plasma-protein bound. If given by subcutaneous or IM injection, plasma concentrations of methylphenidate peaked in about 1 hour a...
Pharmacology of narcotic analgesics in the horse: selective blockade of narcotic-induced locomotor activity.
American journal of veterinary research    May 1, 1981   Volume 42, Issue 5 716-721 
Combie J, Shults T, Nugent EC, Dougherty J, Tobin T.The locomotor responses of horses given morphine and fentanyl were blocked or lessened by administration of naloxone or acepromazine. Naloxone given at the dosage of 0.015 mg/kg completely blocked the locomotor activity induced in horses given fentanyl (0.020 mg/kg of body weight). The locomotor stimulation produced by morphine given at the dosage of 2.4 mg/kg was reduced by 75% of naloxone (0.020 mg/kg). Acepromazine partially blocked the locomotor responses to fentanyl and morphine. This blockade activity reached its peak about 30 minutes after acepromazine was given (IV) and lasted more tha...
Endotoxaemia in the horse.
Equine veterinary journal    April 1, 1981   Volume 13, Issue 2 89-94 doi: 10.1111/j.2042-3306.1981.tb04120.x
Burrows GE.Endotoxins are non-protein fragments of the cell wall of Gram-negative bacteria. They must be absorbed into the circulation to produce disease and systemic effects are similar, regardless of bacterial source. Absorption of endotoxins occurs in obstructive bowel disease and may play a significant part in determining the severity of the disease. Many of the responses to experimentally administered endotoxin are identical to those of bowel diseases or the horse and include circulatory, haematological and metabolic alterations. Therapeutic approaches are indirect and include many drugs currently e...
Aqueous procaine penicillin G in the horse: serum, synovial, peritoneal, and urine concentrations after single-dose intramuscular administration.
American journal of veterinary research    April 1, 1981   Volume 42, Issue 4 629-631 
Stover SM, Brown MP, Kelly RH, Farver TB, Knight HD.Six adult mares were given a single dose of aqueous suspension procaine penicillin G (300,000 IU/ml) IM at a dosage of 22,000 IU/kg of body weight (15.4 mg of penicillin G/kg). Serum, synovial fluid, peritoneal fluid, and urine penicillin concentrations were measured serially over a 48-hour period. The mean peak serum penicillin concentration was 1.42 microgram/ml at 3 hours. Penicillin was detected in synovial fluid and peritoneal fluid, which obtained mean peak penicillin concentrations of 0.62 microgram/ml and 0.58 microgram/ml, at 4 hours and 3 hours, respectively. These concentrations ste...
Resistance to benzimidazole anthelmintics in equine strongyles. 2. Evidence of side-resistance, and susceptibility of benzimidazole-resistant strongyles to non-benzimidazole compounds.
Australian veterinary journal    April 1, 1981   Volume 57, Issue 4 172-181 doi: 10.1111/j.1751-0813.1981.tb00504.x
Webster JH, Baird JD, Gunawan M, Martin IC, Kelly JD.The susceptibility of a known thiabendazole-resistant population of small strongyles to anthelmintics of both benzimidazole and non-benzimidazole groups, was determined. In the first study, 42 horses infected with thiabendazole-resistant small strongyles were allocated to 6 groups. Treatment groups received one of the following anthelmintics: mebendazole, febantel, febantel plus trichlorphon, morantel tartrate, or a combination of thiabendazole, piperazine and trichlorphon. Morantel tartrate and the thiabendazole/piperazine/trichlorphon combination produced highly significant (p less than 0.00...
Effect of aspirin on haemostasis in the horse.
Research in veterinary science    March 1, 1981   Volume 30, Issue 2 241-242 
Judson DG, Barton M.No abstract available
Oxytetracycline hydrochloride in the horse: serum, synovial, peritoneal and urine concentrations after single dose intravenous administration.
Journal of veterinary pharmacology and therapeutics    March 1, 1981   Volume 4, Issue 1 7-10 doi: 10.1111/j.1365-2885.1981.tb00703.x
Brown MP, Stover SM, Kelly RH, Farver TB, Knight HD.Six adult mares were given a single intravenous injection of oxytetracycline HCl (50 mg/ml) at a dosage of 5 mg/kg. Serum, synovial fluid, peritoneal fluid, and urine oxytetracycline concentrations were measured serially over a 48-h period. The highest measured serum oxytetracycline concentration was 8.01 mcg/ml at 1/2 h. Oxytetracycline was detected in synovial fluid and peritoneal fluid, which obtained mean peak oxytetracycline concentrations of 4.43 mcg/ml and 4.20 mcg/ml, at 1/2 h and 1 h, respectively. These concentrations steadily declined in parallel with serum concentrations and were n...
Cardiopulmonary effects of clenbuterol in the horse.
Journal of veterinary pharmacology and therapeutics    March 1, 1981   Volume 4, Issue 1 43-50 doi: 10.1111/j.1365-2885.1981.tb00709.x
Shapland JE, Garner HE, Hatfield DG.Clenbuterol, a bronchospasmolytic agent (beta 2 agonist) was studied in terms of its hemodynamic and airflow response in eight, healthy horses. Four animals were instrumented to record intrapleural pressure and air flow, these were used to compute pulmonary resistance, peak flow rates, and tidal volumes. Four animals were instrumented to record pulmonary arterial pressure, carotid arterial pressure, cardiac output, and arterial gas tensions. After control values were recorded, clenbuterol (0.8 microgram/kg) was intravenously administered to each horse in each experiment group. Following clenbu...
The susceptibility of isolates of Corynebacterium equi to antimicrobial drugs.
Journal of veterinary pharmacology and therapeutics    March 1, 1981   Volume 4, Issue 1 27-31 doi: 10.1111/j.1365-2885.1981.tb00706.x
Prescott JF.Fifty-one isolates of Corynebacterium equi recovered from pigs and horses belonging to two capsular serotypes were tested for susceptibility to antimicrobial agents. No clear differences were detected in sensitivity between isolates of different sources or serotypes. All isolates were sensitive to less than 0.25 micrograms/ml of erythromycin and gentamicin. The following minimum inhibitory concentrations (MICs) of antimicrobial agents were determined for greater than or equal to 90% of isolates: methicillin greater than 16 micrograms/ml, clindamycin 1-2 micrograms/ml, tobramycin less than or e...
Detection of some local anesthetics in horse urine and plasma by gas-liquid chromatography.
Journal of chromatography    February 27, 1981   Volume 206, Issue 3 594-599 doi: 10.1016/s0021-9673(00)88931-1
Delbeke FT, Debackere M, Desmet N.No abstract available
Pharmacokinetics of procaine injected into the hock joint of the horse.
Equine veterinary journal    January 1, 1981   Volume 13, Issue 1 68-69 doi: 10.1111/j.2042-3306.1981.tb03460.x
Wintzer HJ, Fitzek A, Frey HH.No abstract available
[Immobilization of horses with drugs].
Tierarztliche Praxis    January 1, 1981   Volume 9, Issue 2 221-226 
Erbslöh J.No abstract available
Therapeutic effect of phenylbutazone on experimental acute Escherichia coli endotoxemia in ponies.
American journal of veterinary research    January 1, 1981   Volume 42, Issue 1 94-99 
Burrows GE.Phenylbutazone (PBZ), a classic anti-inflammatory and prostaglandin-synthesis inhibitor drug, was used to determine the role of prostaglandins and other mediators on the development and perpetuation of the response to intraperitoneal Escherichia coli endotoxin administration. The PBZ (15 mg/kg of body weight) was administered IV 30 minutes after endotoxin administration and was repeated later at 6 and 12 hours at a dose of 10 mg/kg. A variety of evaluation measurements (hematologic, blood glucose, pyruvate, lactate and fibrinogen, serum beta-glucuronidase, prothrombin time, blood gases, hepati...
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