Smith Joe S, Mochel Jonathan P, Borts David J, Griffith Ronald W
Veterinary Diagnostic and Production Animal Medicine, Iowa State University, Ames, Iowa.
Veterinary Microbiology and Preventive Medicine, Iowa State University, Ames, Iowa.
J Vet Pharmacol Ther. 2019 Jul;42(4):420-429. doi: 10.1111/jvp.12764. Epub 2019 Jun 10.
Tulathromycin is a macrolide antibiotic commonly used for the treatment of respiratory disease in food animal species including goats. Recent research in pigs has suggested that the presence of disease could alter the pharmacokinetics of tulathromycin in animals with respiratory disease. The objectives of this study were (a) compare the plasma pharmacokinetics of tulathromycin in healthy goats as well as goats with an induced respiratory disease; and (b) to compare the tissue residue concentrations of tulathromycin marker in both groups. For this trial, disease was induced with Pasteurella multocida. Following disease induction, tulathromycin was administered. Samples of plasma were collected at various time points up to 312 hr posttreatment, when study animals were euthanized and tissue samples were collected. For PK parameters in plasma, V (control: 28.7 ± 11.9 ml/kg; experimental: 57.8 ± 26.6 ml/kg) was significantly higher (p = 0.0454) in the experimental group than the control group, and nonsignificant differences were noted in other parameters. Among time points significantly lower plasma concentrations were noted in the experimental group at 168 hr (p = 0.023), 216 hr (p = 0.036), 264 hr (p = 0.0017), 288 hr (p = 0.0433), and 312 hr (p = 0.0486). None of the goats had tissue residues above the US bovine limit of 5 µg/g at the end of the study. No differences were observed between muscle, liver, or fat concentrations. A significantly lower concentration (p = 0.0095) was noted in the kidneys of experimental goats when compared to the control group. These results suggest that the effect of respiratory disease on the pharmacokinetics and tissue residues appear minimal after experimental P. multocida infection, however as evidenced by the disparity in C , significant differences in plasma concentrations at terminal time points, as well as the differences in kidney concentrations, there is the potential for alterations in diseased versus clinical animals.
泰拉霉素是一种大环内酯类抗生素,常用于治疗包括山羊在内的食用动物的呼吸道疾病。最近在猪身上的研究表明,疾病的存在可能会改变泰拉霉素在患有呼吸道疾病动物体内的药代动力学。本研究的目的是:(a)比较泰拉霉素在健康山羊和诱发呼吸道疾病山羊体内的血浆药代动力学;(b)比较两组动物体内泰拉霉素标志物的组织残留浓度。在本试验中,用多杀性巴氏杆菌诱发疾病。疾病诱发后,给予泰拉霉素。在治疗后长达312小时的不同时间点采集血浆样本,此时对研究动物实施安乐死并采集组织样本。关于血浆中的药代动力学参数,实验组的V(对照组:28.7±11.9ml/kg;实验组:57.8±26.6ml/kg)显著高于对照组(p = 0.0454),其他参数未发现显著差异。在各时间点中,实验组在168小时(p = 0.023)、216小时(p = 0.036)、264小时(p = 0.0017)、288小时(p = 0.0433)和312小时(p = 0.0486)的血浆浓度显著较低。在研究结束时,没有一只山羊的组织残留量超过美国规定的牛的5μg/g限量。在肌肉、肝脏或脂肪浓度之间未观察到差异。与对照组相比,实验组山羊肾脏中的浓度显著较低(p = 0.0095)。这些结果表明,在实验性多杀性巴氏杆菌感染后,呼吸道疾病对药代动力学和组织残留的影响似乎最小,然而,从血药浓度曲线下面积的差异、终末时间点血浆浓度的显著差异以及肾脏浓度的差异可以看出,患病动物与临床动物相比存在改变的可能性。
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