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肺上皮单层中受体介导的肽递送

Receptor-mediated peptide delivery in pulmonary epithelial monolayers.

作者信息

Deshpande D, Toledo-Velasquez D, Wang L Y, Malanga C J, Ma J K, Rojanasakul Y

机构信息

Department of Basic Pharmaceutical Sciences, School of Pharmacy, West Virginia University, Morgantown 26506.

出版信息

Pharm Res. 1994 Aug;11(8):1121-6. doi: 10.1023/a:1018980630675.

DOI:10.1023/a:1018980630675
PMID:7971712
Abstract

The present study investigated the feasibility of utilizing receptor-mediated endocytosis as a means to enhance peptide delivery to the pulmonary epithelium. The strategy employs a molecular conjugate consisting of a cognate moiety, transferrin (TF), covalently-linked to a model polypeptide, horseradish peroxidase (HRP), via a reversible disulfide linkage. A cultured alveolar epithelial monolayer system was used to simulate the conditions of the pulmonary epithelium and to allow accurate quantitation of intra- and transcellular peroxidase transport. The alveolar cells were isolated from rat lungs by enzymatic digestion and grown on microporous tissue culture-treated polycarbonate filters. A significant increase in the uptake of HRP by the cell monolayer was observed upon its conjugation with TF. The effect was found to be concentration-dependent, being more pronounced at low concentrations, i.e., 3.9- and 1.2-fold increase over unconjugated HRP controls at the concentration levels of 0.05 and 1.50 U/ml respectively. Effective peroxidase uptake was shown to require the TF cognate moiety for the cell surface receptor. Specific internalization of the conjugate by the TF endocytic pathway was verified by competition for the TF receptor. Conjugate internalization was not followed by a proportional increase in transcytosis, i.e., at 0.05 U/ml conjugate level, a 1.7-fold increase in transcytosis was observed as compared to 3.9-fold for endocytosis. Effective enhancement of transcytosis was achieved by treating the monolayers with brefeldin A (BFA), a compound known to affect intracellular transport of TF receptor complexes.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

本研究调查了利用受体介导的内吞作用作为增强肽向肺上皮细胞递送的一种手段的可行性。该策略采用一种分子共轭物,其由一个同源部分转铁蛋白(TF)组成,通过一个可逆的二硫键与一种模型多肽辣根过氧化物酶(HRP)共价连接。使用培养的肺泡上皮单层系统来模拟肺上皮细胞的条件,并准确量化细胞内和跨细胞的过氧化物酶转运。通过酶消化从大鼠肺中分离出肺泡细胞,并在经微孔组织培养处理的聚碳酸酯滤膜上生长。当HRP与TF共轭时,观察到细胞单层对HRP的摄取显著增加。发现该效应具有浓度依赖性,在低浓度时更为明显,即在0.05和1.50 U/ml的浓度水平下,分别比未共轭的HRP对照增加3.9倍和1.2倍。有效的过氧化物酶摄取显示需要TF同源部分与细胞表面受体结合。通过竞争TF受体验证了共轭物通过TF内吞途径的特异性内化。共轭物内化后跨细胞转运并没有成比例增加,即在即0.05 U/ml共轭物水平下,观察到跨细胞转运增加了1.7倍,而内吞作用增加了3.9倍。通过用布雷菲德菌素A(BFA)处理单层细胞实现了跨细胞转运的有效增强,BFA是一种已知会影响TF受体复合物细胞内转运的化合物。(摘要截断于250字)

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