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LLC-PK1A细胞重组成上皮膜过程中Na+/H+反向转运系统的发育与极化

Development and polarization of the Na+/H+ antiport system during reorganization of LLC-PK1A cells into an epithelial membrane.

作者信息

Viniegra S, Rabito C A

机构信息

Department of Radiology, Massachusetts General Hospital, Boston.

出版信息

J Biol Chem. 1988 May 25;263(15):7099-104.

PMID:2835362
Abstract

Changes in Na+/H+ antiport activity and transepithelial electrical resistance were analyzed in a clone of LLC-PK1 cells as the dispersed cells became organized into an epithelial membrane. The clone designated LLC-PK1A showed a 250% increase in Na+/H+ exchange activity as compared with the parent cell line. Na+ influx induced by an outwardly oriented H+ gradient is almost completely abolished during active cell proliferation or after cell dispersion. The activity of the Na+/H+ antiport system increases after plating the cells at high density. This increase precedes the increase in the transepithelial electrical resistance. The increase in the Na+/H+ antiport activity was not observed when the cells were plated at low density in the presence of an antimitotic agent indicating that close cell contact is an absolute requirement for the development of the system. The increase in Na+ influx correlated with an increase in Vmax, while the Km for Na+ remained essentially unchanged. Unidirectional Na+ influx measured from the apical or basolateral side as the dispersed cells became reorganized into an epithelial membrane indicated that the insertion of the Na+/H+ antiporter proteins occurred directly in the apical membrane of the epithelial cells. This finding is consistent with the hypothesis that the sorting of native proteins occurs intracellularly prior to their insertion in the apical membrane of the epithelial cells. The delay in the increase of transepithelial electrical resistance as compared with the increase in Na+ influx indicates that the settlement of the limits between the apical and basolateral membrane (fence function) precedes the closing of the intercellular space (barrier function) during the development of the occluding junctions. Further, the development of the Na+/H+ antiporter was inhibited by cycloheximide but not by actinomycin D, suggesting that the expression of epithelial cell polarization is a translational or posttranslational event.

摘要

在LLC - PK1细胞克隆中,随着分散的细胞组织形成上皮膜,分析了Na⁺/H⁺逆向转运活性和跨上皮电阻的变化。命名为LLC - PK1A的克隆与亲代细胞系相比,Na⁺/H⁺交换活性增加了250%。在活跃的细胞增殖期间或细胞分散后,由外向性H⁺梯度诱导的Na⁺内流几乎完全被消除。将细胞高密度接种后,Na⁺/H⁺逆向转运系统的活性增加。这种增加先于跨上皮电阻的增加。当在抗有丝分裂剂存在的情况下低密度接种细胞时,未观察到Na⁺/H⁺逆向转运活性的增加,这表明紧密的细胞接触是该系统发育的绝对必要条件。Na⁺内流的增加与Vmax的增加相关,而Na⁺的Km基本保持不变。随着分散的细胞重新组织形成上皮膜,从顶端或基底外侧测量的单向Na⁺内流表明,Na⁺/H⁺逆向转运蛋白直接插入上皮细胞的顶端膜。这一发现与以下假设一致,即天然蛋白质的分选在其插入上皮细胞顶端膜之前发生在细胞内。与Na⁺内流的增加相比,跨上皮电阻增加的延迟表明,在紧密连接发育过程中,顶端和基底外侧膜之间界限的形成(栅栏功能)先于细胞间空间的封闭(屏障功能)。此外,环己酰亚胺抑制了Na⁺/H⁺逆向转运蛋白的发育,但放线菌素D没有,这表明上皮细胞极化的表达是一个翻译或翻译后事件。

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