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囊性纤维化黏液模型用于设计更有效的药物疗法。

Cystic Fibrosis Mucus Model to Design More Efficient Drug Therapies.

机构信息

Department of Molecular Biotechnology and Health Science, University of Torino, Via Quarello15, Torino 10135, Italy.

Department of Chemistry, Materials and Chemical Engineering, Giulio Natta-Politecnico di Milano, Piazza Leonardo da Vinci 32, Milano 20133, Italy.

出版信息

Mol Pharm. 2022 Feb 7;19(2):520-531. doi: 10.1021/acs.molpharmaceut.1c00644. Epub 2021 Dec 22.

Abstract

Mucus represents a strong barrier to tackle for oral or pulmonary administered drugs, especially in mucus-related disorders. This study uses a pathological cystic fibrosis (CF) mucus model to investigate how mucus impacts the passive diffusion of 45 commercial drugs selected to maximize physicochemical variability. An mucosal surface was recreated by coupling the mucus model to a 96-well permeable support precoated with structured layers of phospholipids (parallel artificial membrane permeability assay, PAMPA). Results show that the mucus model was not a mere physical barrier but it behaves like an interactive filter. In nearly one-half of the investigated compounds, the diffusion was reduced by mucus, while other drugs were not sensitive to the mucus barriers. We also found that permeability can be enhanced when drug-calcium salts are formed. This was confirmed with cystic fibrosis sputum as a rough model of CF mucus. Since the drug discovery process is characterized by a high rate of failure, the mucus platform is expected to provide an efficient support to early reduce the number of poor-performing drug candidates.

摘要

黏液是口服或肺部给药的药物需要克服的一个强大障碍,尤其是在与黏液相关的疾病中。本研究使用一种病理性囊性纤维化(CF)黏液模型来研究黏液如何影响 45 种商业药物的被动扩散,这些药物是为了最大限度地提高物理化学变异性而选择的。通过将黏液模型与预先涂有磷脂结构化层的 96 孔可渗透载体(平行人工膜渗透性测定法,PAMPA)耦合,重建了黏膜表面。结果表明,黏液模型不仅是一个物理屏障,而且表现得像一个交互式过滤器。在近一半的研究化合物中,扩散被黏液所抑制,而其他药物则不受黏液屏障的影响。我们还发现,当形成药物-钙盐时,渗透性可以增强。这一点通过囊性纤维化痰液作为 CF 黏液的粗糙模型得到了证实。由于药物发现过程的失败率很高,因此该黏液平台有望提供有效的支持,以尽早减少表现不佳的候选药物数量。

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