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豚鼠胃上皮细胞单层需要胶原蛋白IV基质来提供用于生物制药筛选的胃表面的最佳模型。

A collagen IV matrix is required for guinea pig gastric epithelial cell monolayers to provide an optimal model of the stomach surface for biopharmaceutical screening.

作者信息

Kavvada Klairi M, Murray James G, Moore Vanessa A, Coombes Alan G A, Hanson Peter J

机构信息

School of Life and Health Sciences, Aston University, Birmingham, UK.

出版信息

J Biomol Screen. 2005 Aug;10(5):495-507. doi: 10.1177/1087057105276035.

Abstract

The surface epithelial cells of the stomach represent a major component of the gastric barrier. A cell culture model of the gastric epithelial cell surface would prove useful for biopharmaceutical screening of new chemical entities and dosage forms. Primary cultures of guinea pig gastric mucous epithelial cells were grown on filter inserts (Transwells) for 3 days. Tight-junction formation, assessed by transepithelial electrical resistance (TEER) and permeability of mannitol and fluorescein, was enhanced when collagen IV rather than collagen I was used to coat the polycarbonate filter. TEER for cells grown on collagen IV was close to that obtained with intact guinea pig gastric epithelium in vitro. Differentiation was assessed by incorporation of [3H]glucosamine into glycoprotein and by activity of NADPH oxidase, which produces superoxide. Both of these measures were greater for cells grown on filters coated with collagen I than for cells grown on plastic culture plates, but no major difference was found between cells grown on collagens I and IV. The proportion of cells, which stained positively for mucin with periodic acid Schiff reagent, was greater than 95% for all culture conditions. Monolayers grown on membranes coated with collagen IV exhibited apically polarized secretion of mucin and superoxide, and were resistant to acidification of the apical medium to pH 3.0 for 30 min. A screen of nonsteroidal anti-inflammatory drugs revealed a novel effect of diclofenac and niflumic acid in reversibly reducing permeability by the paracellular route. In conclusion, the mucous cell preparation grown on collagen IV represents a good model of the gastric surface epithelium suitable for screening procedures.

摘要

胃表面上皮细胞是胃屏障的主要组成部分。胃上皮细胞表面的细胞培养模型对于新化学实体和剂型的生物制药筛选将被证明是有用的。豚鼠胃黏液上皮细胞的原代培养物在滤膜插入物(Transwells)上生长3天。当使用IV型胶原而非I型胶原包被聚碳酸酯滤膜时,通过跨上皮电阻(TEER)以及甘露醇和荧光素的通透性评估的紧密连接形成得到增强。在IV型胶原上生长的细胞的TEER接近体外完整豚鼠胃上皮所获得的值。通过将[3H]葡萄糖胺掺入糖蛋白以及通过产生超氧化物的NADPH氧化酶的活性来评估分化。对于在I型胶原包被的滤膜上生长的细胞,这两种测量结果均大于在塑料培养板上生长的细胞,但在I型胶原和IV型胶原上生长的细胞之间未发现主要差异。在所有培养条件下,用高碘酸希夫试剂对黏蛋白染色呈阳性的细胞比例均大于95%。在IV型胶原包被的膜上生长的单层细胞表现出黏蛋白和超氧化物的顶端极化分泌,并且对顶端培养基酸化至pH 3.0持续30分钟具有抗性。对非甾体抗炎药的筛选揭示了双氯芬酸和尼氟酸通过细胞旁途径可逆地降低通透性的新作用。总之,在IV型胶原上生长的黏液细胞制剂代表了适合筛选程序的胃表面上皮的良好模型。

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