Disposition kinetics, in vitro plasma protein binding and tissue residues of tilmicosin in healthy and experimentally (CRD) infected broiler chickens

Attia, Taha; Latif, Amera Abd El; El-Hanbally, Saber; El-Gendy, Hanem

doi:10.18203/2319-2003.ijbcp20184328

Cited by 4 publications

(8 citation statements)

References 18 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Regarding of tilmicosin pharmacokinetic after single intracrop administration, the drug was firstly detected at 0.25 h after administration, peaked at 2h post-administration, and decreased gradually till reaching the lowest drug concentration achieved at 24 hr post drug administration. The result of Cmax (1.49 µg/ml), reported in the present study was found to be closely connected to that testified by Attia et al(2018) for tilmicosin in broilers (1.06 µg/ml) and for tilmicosin in rabbits (1.31µg/ml) at 12.5 mg/kg but lower than that stated by Abu-Basha et al(2007) for tilmicosin (Pulmotil AC ® ) in broilers (2.12 μg/ml) at 30 mg/kg, and that reported by Gallina et al,(2010). This discrepancy could be attributed to dose, species differences, and/or the drug assaying process.In contrast, time to peak plasma level (tmax 3.01) was longer compared to that determined by McKay et al (1996) for tilmicosin in rabbits (2h), Abu-Basha et al (2007) for tylosin in chicken (2.36 h), Attia et al (2018) and Shaban et al (2019) for tilmicosin in broilers (2.56h and 2.1h, respectively) but lower than that estimated by Abu-Basha et al (2007) in broilers for tilmicosin (Pulmotil AC ® ) (5.82h) at 30 mg/kg.…”

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 91%

“…The result of Cmax (1.49 µg/ml), reported in the present study was found to be closely connected to that testified by Attia et al(2018) for tilmicosin in broilers (1.06 µg/ml) and for tilmicosin in rabbits (1.31µg/ml) at 12.5 mg/kg but lower than that stated by Abu-Basha et al(2007) for tilmicosin (Pulmotil AC ® ) in broilers (2.12 μg/ml) at 30 mg/kg, and that reported by Gallina et al,(2010). This discrepancy could be attributed to dose, species differences, and/or the drug assaying process.In contrast, time to peak plasma level (tmax 3.01) was longer compared to that determined by McKay et al (1996) for tilmicosin in rabbits (2h), Abu-Basha et al (2007) for tylosin in chicken (2.36 h), Attia et al (2018) and Shaban et al (2019) for tilmicosin in broilers (2.56h and 2.1h, respectively) but lower than that estimated by Abu-Basha et al (2007) in broilers for tilmicosin (Pulmotil AC ® ) (5.82h) at 30 mg/kg. The cause of these differences could be attributed to species and dose variation, medication administration routes, and the presence of food in the chicken crop, which would alter crop motions, as well as the consistency of the feed, which could affect crop emptying.…”

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 91%

“…Following single intracrop administrations of the current investigation, plasma tilmicosin levels in NRI broilers were significantly lower than those in healthy ones. These lower concentrations in infected broilers were consistent with the result formerly stated for tilmicosin by Attia et al (2018) and might be due to the drug's increased penetrating capacity into diseased tissues (Baggot, 1980).Tilmicosin has good tissue penetration and reaches a high concentration and mount up in the lungs of rats than plasma and infection/inflammation further improve its tissue penetration (Modric et al, 1999). This is reliable with the rapid elimination of the drug in diseased birds indicated by the shorter elimination halflife in diseased birds (t½el 8.89h) as compared with the value for healthy ones (t½el 11.32h).…”

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 78%

“…The cause of these differences could be attributed to species and dose variation, medication administration routes, and the presence of food in the chicken crop, which would alter crop motions, as well as the consistency of the feed, which could affect crop emptying. Furthermore, the presence of lactobacillus flora in the crop, which may be responsible for macrolide inactivation (Cerda et al, 2010).Tilmicosin was rapidly absorbed, with a short absorption half-life (t0.5ab, 0.59 h), similar to what Abo- El-Sooud et al (2012) found for azithromycin in broiler chickens (t0.5ab 0.57h), Attia et al, (2018) for tilmicosin in broiler chickens (0.52 hr) but shorter than those stated by Li (2003) for tilmicosin in broilers (0.948h and 0.757h) and that reported by Shu et al (2004) for tilmicosin in chicken (0.66h) which could be due to individual differences (Cerda et al, 2010). Tilmicosin has been gradually eliminated with elimination half-life (t0.5el 11.32 h).This result is closely connected to that reported by Shaban et al (2019) for tilmicosin in broilers (13.49 hours), but lower than those recorded for tilmicosin in chicken (30.18, 24.18, 47.4, and 21.86 hours) as determined by Keles et al (2001); Li (2003); Abu-Basha et al, (2007); Attia et al, (2018), respectively.…”

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 57%

See 3 more Smart Citations

Tilmicosin Pharmacokinetics and Tissue Residues in Healthy and Naturally Respiratory Infected Broilers

Attia

El-Banna

Selim³

et al. 2021

Journal of Current Veterinary Research

Self Cite

View full text Add to dashboard Cite

The goal of this study was to clarify the tilmicosin pharmacokinetics in healthy and naturally infected broiler with respiratory disorders (NRI). Tilmicosin achieved its Cmax after 3.01 and 2.63 h (Tmax) of administration, with values of 1.21 and 0.93 µg/ml, respectively, following single intracrop dose (25 mg/kg BW). Tilmicosin t0.5ab was 0.590.034 h & 0.590.02 h and t0.5el was 011.32 & 8.89 h, sequentially. Tilmicosin attained its Cmax following a single intramuscular injection (25 mg/kg BW, IM) after 1.51 & 1.56 h (Tmax), respectively, with values of 1.20 and 1.28 µg/ml. The t0.5ab (0.29 & 0.30 h) and t0.5el (7.07 & 5.04 h) of tilmicosin showed a clear reduction relative to intracrop dosing, serially. Tissue residues after repeated oral (75 mg/L of drinking water for 3 consecutive days) administration revealed a lower significant plasma tilmicosin concentration after all times of sampling in NRI chickens related to those of healthy ones. Tilmicosin residues was assayed in lung, kidney, liver, thigh and breast muscles, after "2h, 24 h, 3d, 5d, 7d, 9d and 11 days post tilmicosin stoppage. The highest residue values were found in the lungs, followed by the liver and kidneys, while the lowest irrelevant values were found in the thigh and breast muscles. Finally, tilmicosin has a fast absorption rate, a long elimination half-life, and substantial bloodto-tissue penetration, particularly in the lungs. Following repeated oral tilmicosin administration, the required withdrawal period is 9 d for thigh and breast muscles and 10 d for internal organs.

show abstract

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 91%

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 91%

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 78%

Section: Pharmacokinetic Of Single Intracrop Tilmicosin Administration In Healthy and Nri Broilerssupporting

confidence: 57%

See 2 more Smart Citations

Tilmicosin Pharmacokinetics and Tissue Residues in Healthy and Naturally Respiratory Infected Broilers

Attia

El-Banna

Selim³

et al. 2021

Journal of Current Veterinary Research

Self Cite

View full text Add to dashboard Cite

show abstract

“…These findings were in concordance with those of Salman et al (2016) who reported that the serum concentrations of tylvalosin was significantly lower in M. gallisepticum infected chickens compared to healthy ones. Similarly, Attia et al (2018) mentioned that the serum levels of tilmicosin were markedly higher in healthy chickens than in M. gallisepticum and Escherichia coli infected ones.…”

Section: Discussionmentioning

confidence: 97%

Pharmacokinetics of Tildipirosin in Healthy and Mycoplasma gallisepticum Infected Chickens

2021

Int J Vet Sci

View full text Add to dashboard Cite

The pharmacokinetic features of tildipirosin were explored following a single dose of 4 mg/kg in healthy and Mycoplasma gallisepticum (M. gallisepticum) infected chickens. Eighteen healthy chickens (400-500g) were allocated into 3 groups (n=6); group I and II were received tildipirosin by intravenous (IV) and intramuscular (IM) routes, respectively. Group III was experimentally infected with M. gallisepticum and injected IM with tildipirosin after confirming the infection (9-10 days after inoculation of M. gallisepticum). Plasma samples were harvested at different time points until 14 days after tildipirosin injection to measure its concentrations using HPLC. After IM administration of tildipirosin in healthy chickens, the maximum concentration in plasma (Cmax), time to achieve Cmax (Tmax), area under the plasma concentration time curve from 0 to last time (AUC0-last), clearance (Cl-F-obs) and the absolute bioavailability were recorded to be 403.76ng/ml, 0.25 hr, 6.82 µg.hr/ml, 0.56L/hr/kg, and 103.50% respectively. Cmax and AUC0-last, were significantly lower in infected than healthy chickens, while Cl-F-obs was significantly higher in infected than healthy chickens. Therefore, M. gallispeticum infection produced significant changes in some of the pharmacokinetic parameters of tildipirosin in chickens. Further studies are warranted to assess pharmacokinetic/ pharmacodynamic profile of tildipirosin against M. gallisepticum in chickens and to gain deeper insight into its safety utilization in chickens.

show abstract

Intake and distribution of doxycycline in the organism of broiler chickens

Tyshkivskaya

Dukhnytskyi

Tyshkivsky

2020

Nauk. vìsn. vet. med.

View full text Add to dashboard Cite

The article presents the results of studies on the absorption, distribution and excretion of the antibiotic Poledoxin (the active substance is doxycycline hyclact) from the body of healthy broiler chickens of the Koob-500 cross when taken orally. Studies have established the rapid absorption of doxycycline hyclact from the digestive tract of the chicken into the blood and its entry into the internal organs. The maximum concentration of doxycycline hyclact was detected 2-4 hours after the start of Poledoxin administration, the content of which in the liver was 9,07±0,07 μg/g, in the lungs – 8,39±0,20 μg/g, in the heart – 4,24±0,09 μg/g, in the pectoral muscles – 4,28±0,23 μg/g. In the kidneys, the maximum concentration was found after 12 hours – 7,63±0,38 μg/g. When clinically healthy broiler chickens were fed with Poledoxin solution, the ability to materially cumulate doxycycline hyclact (active ingredient) was not established, since its content in the internal organs and muscles of the bird did not depend on the duration of the drug use. Studies have established the absence of organ affiliation of doxycycline hyclact, because its maximum content, depending on the study period, was recorded in various organs that provide biotransformation and excretion – liver, kidneys, lungs. The cancellation of drinking Poledoxin ensured the rapid elimination of doxycyclin hyclact from the body of broiler chickens and, after 5 days (for 216 hours of the experiment), its content was minimal for the entire study period and amounted to: in the kidneys – 0,15±0,01 μg/g; liver – 0,12±0,01 μg/g; pectoral muscles – 0,05±0,01 μg/g; lungs – 0,04±0,01 μg/g. Only in one sample of the heart, doxycycline hyclact was shown in an amount of 0,01 μg/g. Key words: Poledoxin, doxycycline hyclact, broiler chickens, distribution, accumulation, hatching, bioavailability, pharmacokinetics, excretion.

show abstract

Disposition kinetics, in vitro plasma protein binding and tissue residues of tilmicosin in healthy and experimentally (CRD) infected broiler chickens

Cited by 4 publications

References 18 publications

Tilmicosin Pharmacokinetics and Tissue Residues in Healthy and Naturally Respiratory Infected Broilers

Tilmicosin Pharmacokinetics and Tissue Residues in Healthy and Naturally Respiratory Infected Broilers

Pharmacokinetics of Tildipirosin in Healthy and Mycoplasma gallisepticum Infected Chickens

Intake and distribution of doxycycline in the organism of broiler chickens

Contact Info

Product

Resources

About