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切除的牛鼻黏膜作为体外模型用于研究鼻上皮中药物转运和代谢途径的验证。

Validation of excised bovine nasal mucosa as in vitro model to study drug transport and metabolic pathways in nasal epithelium.

作者信息

Schmidt M C, Simmen D, Hilbe M, Boderke P, Ditzinger G, Sandow J, Lang S, Rubas W, Merkle H P

机构信息

Department of Applied BioSciences, Swiss Federal Institute of Technology Zurich (ETH), Winterthurerstrasse 190, 8057 Zurich, Switzerland.

出版信息

J Pharm Sci. 2000 Mar;89(3):396-407. doi: 10.1002/(SICI)1520-6017(200003)89:3<396::AID-JPS10>3.0.CO;2-F.

Abstract

The present work aims at the validation of excised bovine nasal mucosa as an in vitro model to address transport and metabolism pathways relative to the nasal mucosal uptake of therapeutic peptides. Preservation of the viability of the excised tissue in the course of in vitro studies of up to 3 h was demonstrated by (i) positive viability staining, (ii) constant transepithelial electrical resistance (42 +/- 12 Omega cm(2)), (iii) constant rates of metabolic turnover, and (iv) linear permeation profiles of therapeutic peptides and (3)H-mannitol. Using 1-leucine-4-methoxy-2-naphthylamide as a model substrate, we observed no difference between bovine and human nasal aminopeptidase activity. By a series of therapeutic peptides, no direct correlation was found between their effective permeability coefficients (from 0. 1 x 10(-5) to 5 x 10(-5) cm s(-1)) and their respective molecular masses (from 417 to 3,432 Da), indicating that other factors dominate nasal permeability. For instance, the permeabilities of metabolically labile peptides were concentration dependent and saturable, as demonstrated for two short thymopoietin fragments, Arg-Lys-Asp (TP3) and Arg-Lys-Asp-Val (TP4). By permeation studies using gonadorelin and two gonadorelin derivatives, buserelin and Hoe 013, without and in the presence of the chemical enhancer bacitracin, we also verified the ability of the model to assess chemical enhancer effects and their reversibility. In conclusion, our work demonstrates the potential of the investigated in vitro model, excised bovine nasal mucosa, to explore mechanistic aspects of nasal transport and metabolism of therapeutic peptides.

摘要

本研究旨在验证切除的牛鼻黏膜作为体外模型,以研究与治疗性肽经鼻黏膜摄取相关的转运和代谢途径。在长达3小时的体外研究过程中,切除组织的活力通过以下方式得以证实:(i) 活力染色呈阳性;(ii) 跨上皮电阻恒定(42±12Ω·cm²);(iii) 代谢周转率恒定;(iv) 治疗性肽和³H-甘露醇的渗透曲线呈线性。以1-亮氨酸-4-甲氧基-2-萘酰胺作为模型底物,我们观察到牛和人鼻氨肽酶活性之间没有差异。对于一系列治疗性肽,未发现它们的有效渗透系数(从0.1×10⁻⁵至5×10⁻⁵cm/s)与各自的分子量(从417至3432Da)之间存在直接相关性,这表明其他因素主导鼻通透性。例如,对于两个短的胸腺生成素片段,精氨酸-赖氨酸-天冬氨酸(TP3)和精氨酸-赖氨酸-天冬氨酸-缬氨酸(TP4),代谢不稳定肽的通透性具有浓度依赖性且可饱和。通过使用促性腺激素释放激素以及两种促性腺激素释放激素衍生物布舍瑞林和Hoe 013进行渗透研究,在不存在和存在化学增强剂杆菌肽的情况下,我们还验证了该模型评估化学增强剂效果及其可逆性的能力。总之,我们的研究证明了所研究的体外模型——切除的牛鼻黏膜,在探索治疗性肽经鼻转运和代谢的机制方面的潜力。

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