Effect of Ketoprofen on acute phase protein concentrations in goats undergoing castration

Karademir, Umit; Akin, Ibrahim; Erdoğan, Hasan; Ural, Kerem; Aşıcı, Gamze Sevri Ekren

doi:10.1186/s12917-016-0748-y

Cited by 6 publications

(12 citation statements)

References 38 publications

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“…Clinical use of firocoxib would most likely occur in nonfasted animals, and, as such, the pharmacokinetics in unfasted goats likely represent the clinical application of firocoxib. The mean half‐life of oral firocoxib in this study, 21.5 hr, was much longer than those reported for oral meloxicam and oral flunixin in goats at 10.7–11.8 hr [mean] and 4.2 hr [median], respectively (Ingvast‐Larsson et al, ; Karademir, Akin, et al, ; Karademir, Erdogan, et al, ; Konigsson et al, ) (Table ). This prolonged half‐life may result in dose accumulation with subsequent doses, depending on dosing interval.…”

Section: Discussionmentioning

confidence: 47%

“…Bioavailability of oral firocoxib was relatively high with a mean of 71%. Mean bioavailability of oral meloxicam in goats has previously been found to be between 79% and 96% (Ingvast‐Larsson et al, ; Karademir, Akin, et al, ; Karademir, Erdogan, et al, ), while the median bioavailability of orally administered flunixin meglumine was lower at 58% (Konigsson, Torneke, Engeland, Odensvik, & Kindahl, ) (Table ). These results indicate good absorption following oral administration of firocoxib, despite the goats' unfasted state, and suggest that absorption is similar to that of other studied NSAIDs.…”

Section: Discussionmentioning

confidence: 98%

“…The concentration of firocoxib was undetectable (<5 ng/ml) at time 0 for both treatment groups, indicating that no goat had received firocoxib prior to the start of the study period and that the 14‐day washout period was adequate. The mean time to maximal concentration following oral firocoxib administration was less than an hour, representing more rapid absorption when compared to oral meloxicam (Ingvast‐Larsson et al, ; Karademir, Akin, et al, ; Karademir, Erdogan, et al, ) in goats (Table ). Bioavailability of oral firocoxib was relatively high with a mean of 71%.…”

Section: Discussionmentioning

confidence: 99%

“…The dose was rounded to the nearest 0.01 g of paste. This dose was selected based on pharmacokinetic studies of other NSAIDs in goats and other ruminants (Ingvast‐Larsson et al, ; Karademir, Akin, et al, ; Karademir, Erdogan, et al, ; Stock et al, , ).…”

Section: Methodsmentioning

confidence: 99%

“…Animal welfare and pain management in livestock species have become increasingly prevalent topics of discussion and study for producers, veterinarians, and society (Fraser et al, ; Grandin, ; Phillips, Wojciechowska, Meng, & Cross, ; Shivley, Garry, Kogan, & Grandin, ). Researchers have attempted to provide evidence of beneficial effects of analgesia for routine procedures such as disbudding and castration in cattle (Coetzee, ; Stock, Baldridge, Griffin, & Coetzee, ) and small ruminants (Ingvast‐Larsson et al, ; Karademir, Akin, Akin, Erdogan, Ural, & Asici, ; Karademir, Erdogan, et al, ). Long‐term pain management is also important for the welfare of production and pet goats alike, and examples of conditions where chronic pain medication may be indicated include osteoarthritis (either primary or secondary to infection with caprine arthritis encephalitis virus), fracture, spondylitis, foot rot and abscesses, corneal ulceration, and postoperative pain (Anderson & Muir, ; Galatos, ; Plummer & Schleining, ).…”

Section: Introductionmentioning

confidence: 99%

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Pharmacokinetics and bioavailability of oral firocoxib in adult, mixed‐breed goats

Stuart

KuKanich

Caixeta

et al. 2019

Vet Pharm & Therapeutics

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Pharmacokinetic (PK) studies of oral firocoxib in large animal species have been limited to horses, preruminating calves, and adult camels. The aim of this study was to describe pharmacokinetics and bioavailability of firocoxib in adult goats. Ten healthy adult goats were administered 0.5 mg/kg firocoxib intravenously (i.v.) and per os (p.o.) in a randomized, crossover study. Plasma firocoxib concentrations were measured over a 96‐hr period for each treatment using HPLC and mass spectrometry, and PK analysis was performed. The p.o. formulation reached mean peak plasma concentration of 139 ng/ml (range: 87–196 ng/ml) in 0.77 hr (0.25–2.00 hr), and half‐life was 21.51 hr (10.21–48.32 hr). Mean bioavailability was 71% (51%–82%), indicative of adequate gastrointestinal absorption of firocoxib. There were no negative effects observed in any animal, and all blood work values remained within or very near reference range at the study's conclusion. Results indicate that oral firocoxib is well‐absorbed and rapidly reaches peak plasma concentrations, although the concentration also decreased quickly prior to the terminal phase. The prolonged half‐life may suggest tissue accumulation and higher plasma concentrations over time, depending on dosing schedule. Further studies to determine tissue residue depletion, pharmacodynamics, and therapeutic concentrations of firocoxib in goats are necessary.

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Section: Discussionmentioning

confidence: 47%

Section: Discussionmentioning

confidence: 98%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Pharmacokinetics and bioavailability of oral firocoxib in adult, mixed‐breed goats

Stuart

KuKanich

Caixeta

et al. 2019

Vet Pharm & Therapeutics

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Using systemic serum amyloid A as a biomarker for synovial structure infections in horses with acute limb wounds

2022

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Background: In postoperative monitoring of synovial structure infection due to limb wounds, early recognition of a recurrence of synovial infection is indispensable to prevent further damage to the affected synovial structure. This study evaluated the role of serum amyloid A (SAA) as a systemic biomarker in disease monitoring and correlated this tool with clinical variables. Methods: In this prospective cohort study, 55 horses with acute limb wounds were divided into two groups: those with (group 1, n = 26) or without (group 2, n = 29) a diagnosis of synovial structure penetration. SAA, lameness and body temperature were evaluated repeatedly and compared between groups. Correlations were explored between SAA and body temperature as well as lameness. The long-term outcome was also analysed. Results: In both groups, SAA levels followed the characteristic rise-and-fall pattern observed in previous studies, with a significant increase up to a peak concentration within 48 hours, followed by a constant decline. Lameness and body temperature did not change significantly. SAA was not found to correlate with clinical variables at all time points. Three horses in group 1 had a recurrence of synovial sepsis with an associated increase in SAA. The longterm outcome was good. A total of 71% of the study population returned to pre-injury performance levels. Conclusion: Repeated measurements of SAA accurately reflected the course of synovial inflammation and thus provided a reliable and rapidly available tool to monitor the disease course and to adapt the treatment regimen. SAA should be routinely added to the postoperative management of such cases.

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Can blood serum amyloid A concentrations in horses differentiate synovial sepsis from extrasynovial inflammation and determine response to treatment?

Sinovich

Villarino

Singer³

et al. 2020

Veterinary Record

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BackgroundSerum amyloid A (SAA) concentrations in blood and synovial fluid of horses with synovial sepsis have diagnostic value. Studies suggest serial blood SAA measurements could act as a prognostic indicator. This study evaluated the use of serial blood SAA concentrations for monitoring of horses with synovial sepsis.MethodsA prospective clinical trial was performed of horses referred to a single hospital with synovial sepsis that survived (n=17), synovial sepsis that were euthanised (n=5), non-septic intrasynovial pathologies (n=14) or extensive extrasynovial lacerations (n=5). SAA concentrations were determined on admission and every 24 hours thereafter. The area under the concentration–time curve from 0 to 144 hours of each group was compared by Kruskal-Wallis and post hoc Dunn’s tests (P<0.05).ResultsSignificant difference in mean blood concentration of SAA was found between synovial sepsis that survived and non-septic pathologies in the first 48 hours, as well as between non-septic intrasynovial pathologies and non-responsive sepsis requiring euthanasia. No difference was found between extensive extrasynovial lacerations and any septic group.ConclusionsWhile serial blood SAA is useful for monitoring clinical response of intrasynovial septic pathologies, interpretation should consider other clinical findings since blood SAA is not a specific marker for synovial sepsis.

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Effect of Ketoprofen on acute phase protein concentrations in goats undergoing castration

Cited by 6 publications

References 38 publications

Pharmacokinetics and bioavailability of oral firocoxib in adult, mixed‐breed goats

Pharmacokinetics and bioavailability of oral firocoxib in adult, mixed‐breed goats

Using systemic serum amyloid A as a biomarker for synovial structure infections in horses with acute limb wounds

Can blood serum amyloid A concentrations in horses differentiate synovial sepsis from extrasynovial inflammation and determine response to treatment?

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