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转染内皮细胞和上皮细胞中聚合免疫球蛋白受体的反向分选和转胞吞作用

Opposite sorting and transcytosis of the polymeric immunoglobulin receptor in transfected endothelial and epithelial cells.

作者信息

Su T, Stanley K K

机构信息

The Heart Research Institute, Camperdown, NSW 2050, Sydney, Australia.

出版信息

J Cell Sci. 1998 May;111 ( Pt 9):1197-206. doi: 10.1242/jcs.111.9.1197.

Abstract

We have transfected a polarised endothelial cell line, ECV 304, and an epithelial cell line, MDCK, with a well characterised epithelial protein, the rat polymeric immunoglobulin receptor (pIgR), in order to study the protein sorting and transcytosis in endothelial cells. The expressed protein was normally processed and the steady state distribution between apical and basolateral surfaces was similar in both cell types. MDCK cells, however, showed a marked polarity in the delivery of newly synthesised pIgR to the cell surface, and in the release of secretory component. 88% of newly synthesised pIgR in MDCK cells was first delivered to the basolateral surface and 99% of secretory component was released from the apical surface. In contrast the basolateral targeting signal of pIgR was only partially recognised in endothelial cells, with 63% of the newly synthesised pIgR being first delivered to the basolateral surface. At steady state only 43% of the pIgR was found on the basolateral membrane. The direction of dimeric IgA transcytosis in endothelial cells was from apical to basolateral surfaces, opposite to that in MDCK cells. These data suggest that endothelial cells poorly recognise the targeting signals of proteins from epithelial cells, and that the direction of transcytosis is linked to the biological role of the cells.

摘要

为了研究内皮细胞中的蛋白质分选和转胞吞作用,我们用一种特征明确的上皮蛋白——大鼠多聚免疫球蛋白受体(pIgR)转染了极化内皮细胞系ECV 304和上皮细胞系MDCK。表达的蛋白正常加工,两种细胞类型中顶端和基底外侧表面的稳态分布相似。然而,MDCK细胞在将新合成的pIgR递送至细胞表面以及分泌成分的释放方面表现出明显的极性。MDCK细胞中88%新合成的pIgR首先被递送至基底外侧表面,99%的分泌成分从顶端表面释放。相比之下,pIgR的基底外侧靶向信号在内皮细胞中仅被部分识别,63%新合成的pIgR首先被递送至基底外侧表面。在稳态时,仅43%的pIgR存在于基底外侧膜上。内皮细胞中二聚体IgA转胞吞作用的方向是从顶端表面到基底外侧表面,与MDCK细胞相反。这些数据表明内皮细胞对上皮细胞来源蛋白质的靶向信号识别较差,并且转胞吞作用的方向与细胞的生物学作用相关。

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