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Modulation of fodrin (membrane skeleton) stability by cell-cell contact in Madin-Darby canine kidney epithelial cells

机译:Madin-Darby犬肾上皮细胞中细胞间接触对铁蛋白(膜骨架)稳定性的调节

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摘要

During growth of Madin-Darby canine kidney (MDCK) epithelial cells, there is a dramatic change in the stability, biophysical properties, and distribution of the membrane skeleton (fodrin) which coincides temporally and spatially with the development of the polarized distribution of the Na+, K+-ATPase, a marker protein of the basolateral domain of the plasma membrane. These changes occur maximally upon the formation of a continuous monolayer of cells, indicating that extensive cell-cell contact may play an important role in the organization of polarized MDCK cells (Nelson, W. J., and P. J. Veshnock, 1986, J. Cell Biol., 103:1751-1766). To directly analyze the role of cell-cell contact in these events, we have used an assay in which the organization of fodrin and membrane proteins is analyzed in confluent monolayers of MDCK cells in the absence or presence of cell-cell contact by adjusting the concentration Ca++ in the growth medium. Our results on the stability and solubility properties of fodrin reported here show directly that there is a positive correlation between cell- cell contact and increased stability and insolubility of fodrin. Furthermore, we show that fodrin can be recruited from an unstable pool of protein to a stable pool during induction of cell-cell contact; significantly, the stabilization of fodrin is not affected by the addition of cyclohexamide, indicating that proteins normally synthesized during the induction of cell-cell contact are not required. Together these results indicate that cell-cell contact may play an important role in the development of polarity in MDCK cells by initiating the formation of a stable, insoluble matrix of fodrin with preexisting (membrane) proteins at the cell periphery. This matrix may function subsequently to trap proteins targeted to the membrane, resulting in the maintenance of membrane domains.
机译:在Madin-Darby犬肾(MDCK)上皮细胞生长期间,其稳定性,生物物理特性和膜骨架(fodrin)的分布发生了巨大变化,这在时间和空间上与Na +极化分布的发展相吻合。 ,K + -ATPase,质膜基底外侧结构域的标记蛋白。这些变化在形成连续的单层细胞时最大程度地发生,表明广泛的细胞间接触可能在极化的MDCK细胞的组织中起重要作用(Nelson,WJ和PJ Veshnock,1986,J.Cell Biol。, 103:1751-1766)。为了直接分析细胞-细胞接触在这些事件中的作用,我们使用了一种分析方法,其中通过调节浓度来分析在不存在或存在细胞-细胞接触的情况下,MDCK细胞的融合单层中的铁蛋白和膜蛋白的组织。 Ca ++在生长培养基中。我们在此报道的关于铁蛋白的稳定性和溶解性的结果直接表明,细胞间接触与铁蛋白的稳定性和不溶性增加之间存在正相关关系。此外,我们表明,在诱导细胞与细胞接触的过程中,铁蛋白可以从不稳定的蛋白质池中募集到稳定的池中。明显地,添加环己酰胺不会影响草精的稳定,这表明不需要诱导细胞-细胞接触过程中正常合成的蛋白质。这些结果共同表明,细胞与细胞之间的接触可能通过启动稳定的,不溶的铁蛋白与在细胞外围存在的(膜)蛋白的稳定形成而在MDCK细胞的极性发展中发挥重要作用。该基质可随后起作用以捕获靶向膜的蛋白质,从而维持膜结构域。

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