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Mucosal permeability of water-soluble drugs in the equine jejunum: a preliminary investigation

机译:空肠内水溶性药物的粘膜渗透性:初步研究

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Ussing chambers have been used to study the mucosal permeability of drugs in humans, rats and other species. This data can then be used to develop in vitro/in vivo correlations (IVIVC) for drugs based on the Biopharmaceutics Classification System (BCS). Due to the poor oral bioavailability of many drugs in the horse, this method may be useful for screening drugs before development to determine if they warrant further study. Cephalexin (CPX), marbofloxacin (MAR), metronidazole (MTZ) and fluconazole (FCZ) were chosen for this study based on the wide range of physicochemical properties and bioavailability in the horse. Permeability was ranked as follows: MTZ FCZ MAR CPX. This correlated with the bioavailability (R(2) = 0.633447), the Log P (R(2) = 0.648517), as well as the molecular weight (R(2) = 0.851208) of the drugs. Metronidazole induced a decrease in the tissue transepithelial resistance, suggestive of the possibility of tissue toxicity, which may have falsely increased its permeability. The low permeability of cephalexin across the tissue may indicate a lack of active transporters that are found in other species. From this study, we can conclude that the Ussing chamber is a promising method for determining mucosal permeability in the horse.
机译:Ussing chambers已用于研究药物在人,大鼠和其他物种中的粘膜渗透性。然后,可以基于生物制药分类系统(BCS)将这些数据用于开发药物的体外/体内相关性(IVIVC)。由于许多药物在马中的口服生物利用度较差,因此该方法可用于在药物开发之前进行筛查以确定是否需要进一步研究。基于广泛的理化特性和马匹的生物利用度,本研究选择了头孢氨苄(CPX),马波沙星(MAR),甲硝唑(MTZ)和氟康唑(FCZ)进行此项研究。渗透性排名如下:MTZ> FCZ> MAR> CPX。这与药物的生物利用度(R(2)= 0.633447),Log P(R(2)= 0.648517)以及分子量有关(R(2)= 0.851208)。甲硝唑引起组织​​跨上皮抵抗力降低,提示组织毒性的可能性,这可能会错误地增加其通透性。头孢氨苄在整个组织中的低渗透性可能表明缺乏其他物种中发现的活性转运蛋白。从这项研究中,我们可以得出结论:“前驱室”是一种确定马黏膜通透性的有前途的方法。

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