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首页> 外文期刊>Medical mycology: official publication of the International Society for Human and Animal Mycology >A model for treating avian aspergillosis: Serum and lung tissue kinetics for Japanese quail (Coturnix japonica) following single and multiple aerosol exposures of a nanoparticulate itraconazole suspension
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A model for treating avian aspergillosis: Serum and lung tissue kinetics for Japanese quail (Coturnix japonica) following single and multiple aerosol exposures of a nanoparticulate itraconazole suspension

机译:一种治疗禽曲霉病的模型:一次或多次暴露于纳米微粒伊曲康唑悬浮液中的日本鹌鹑(Coturnix japonica)的血清和肺组织动力学

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摘要

Aspergillosis is frequently reported in parrots, falcons and other birds held in captivity. Inhalation is the main route of infection for Aspergillus fumigatus, resulting in both acute and chronic disease conditions. Itraconazole (ITRA) is an antifungal commonly used in birds, but administration requires repeated oral dosing and the safety margin is narrow. We describe lung tissue and serum pharmacokinetics of a nanoparticulate ITRA suspension administered to Japanese quail by aerosol exposure. Aerosolized ITRA (1 and 10% suspension) administered over 30 min did not induce adverse clinical reactions in quail upon single or 5-day repeated doses. High lung concentrations, well above the inhibitory levels for A. fumigatus, of 4.14 ± 0.19 μg/g and 27.5 ± 4.58 μg/g (mean ± SEM, n = 3), were achieved following single-dose inhalation of 1% and 10% suspension, respectively. Upon multiple dose administration of 10% suspension, mean lung concentrations reached 104.9 ± 10.1 μg/g. Drug clearance from the lungs was slow with terminal half-lives of 19.7 h and 35.8 h following inhalation of 1% and 10% suspension, respectively. Data suggest that lung clearance is solubility driven. Lung concentrations of hydroxy-itraconazole reached 1-2% of the ITRA lung tissue concentration indicating metabolism in lung tissue. Steady, but low, serum concentrations of ITRA could be measured after multiple dose administration, reaching less than 0.1% of the lung tissue concentration. This formulation may represent a novel, easy to administer treatment modality for fungal lung infection, preventing high systemic exposure. It may also be useful as metaphylaxis to prevent the outbreak of aspergillosis in colonized animals.
机译:鹦鹉,猎鹰和其他人工饲养的鸟类经常报道曲霉病。吸入是烟曲霉的主要感染途径,可导致急性和慢性疾病。伊曲康唑(ITRA)是禽类常用的抗真菌药,但给药需要反复口服,安全性差。我们描述了通过喷雾暴露给日本鹌鹑的纳米ITRA悬浮液的肺组织和血清药代动力学。在单次或5天重复剂量下,在30分钟内施用的雾化ITRA(1%和10%悬浮液)不会引起鹌鹑的不良临床反应。单次吸入1%和10剂量后,获得了较高的肺部浓度,分别高于烟曲霉的抑制水平4.14±0.19μg/ g和27.5±4.58μg/ g(平均值±SEM,n = 3)。分别为%悬浮液。多次给药10%悬浮液后,平均肺部浓度达到104.9±10.1μg/ g。分别吸入1%和10%悬浮液后,从肺部清除药物的速度很慢,终末半衰期分别为19.7小时和35.8小时。数据表明肺清除率是溶解度驱动的。肺中羟基伊曲康唑的浓度达到ITRA肺组织浓度的1-2%,表明在肺组织中代谢。多次给药后,可以测定稳定但低的ITRA血清浓度,达到肺组织浓度的0.1%以下。该制剂可以代表新颖的,易于施用的用于真菌性肺部感染,防止高全身暴露的治疗方式。它也可以用作预防在定植动物中曲霉病暴发的代谢药物。

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