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Membrane domains of intestinal epithelial cells: distribution of Na+,K+- ATPase and the membrane skeleton in adult rat intestine during fetal development and after epithelial isolation

机译:肠道上皮细胞的膜结构域:胎儿发育过程中和上皮分离后成年大鼠肠中Na +,K +-ATPase和膜骨架的分布

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摘要

The organization of the basolateral membrane domain of highly polarized intestinal absorptive cells was studied in adult rat intestinal mucosa, during development of polarity in fetal intestine, and in isolated epithelial sheets. Semi-thin frozen sections of these tissues were stained with a monoclonal antibody (mAb 4C4) directed against Na+,K+- ATPase, and with other reagents to visualize distributions of the membrane skeleton (fodrin), an epithelial cell adhesion molecule (uvomorulin), an apical membrane enzyme (aminopeptidase), and filamentous actin. In intact adult epithelium, Na+,K+-ATPase, membrane- associated fodrin, and uvomorulin were concentrated in the lateral, but not basal, subdomain. In the stratified epithelium of fetal intestine, both fodrin and uvomorulin were localized in areas of cell-cell contact at 16 and 17 d gestation, a stage when Na+,K+-ATPase was not yet expressed. These molecules were excluded from apical domains and from cell surfaces in contact with basal lamina. When Na+,K+-ATPase appeared at 18-19 d, it was codistributed with fodrin. Detachment of epithelial sheets from adult intestinal mucosa did not disrupt intercellular junctions or lateral cell contacts, but cytoplasmic blebs appeared at basal cell surfaces, and a diffuse pool of fodrin and actin accumulated in them. At the same time, Na+,K+-ATPase moved into the basal membrane subdomain, and extensive endocytosis of basolateral membrane, including Na+,K+-ATPase, occurred. Endocytosis of uvomorulin was not detected and no fodrin was associated with endocytic vesicles. Uvomorulin, along with some membrane-associated fodrin and some Na+,K+-ATPase, remained in the lateral membrane as long as intercellular contacts were maintained. Thus, in this polarized epithelium, interaction of lateral cell-cell adhesion molecules as well as basal cell-substrate interactions are required for maintaining the stability of the lateral membrane skeleton and the position of resident membrane proteins concentrated in the lateral membrane domain.
机译:在成年大鼠肠道粘膜中,胎儿肠道中的极性形成过程中以及在分离的上皮层中研究了高度极化的肠道吸收性细胞的基底外侧膜结构域的组织。用针对Na +,K +-ATPase的单克隆抗体(mAb 4C4)和其他试剂对这些组织的半薄冰冻切片进行染色,以可视化膜骨架(fodrin),上皮细胞粘附分子(umormorulin)的分布,顶端膜酶(氨肽酶)和丝状肌动蛋白。在完整的成年上皮细胞中,Na +,K + -ATPase,膜相关的铁蛋白和葡萄膜蛋白被集中在外侧而不是基底子域中。在胎儿肠的分层上皮中,在妊娠16和17天时,铁蛋白和葡萄胎蛋白都定位在细胞与细胞接触的区域,这是Na +,K + -ATPase尚未表达的阶段。这些分子被排除在顶端区域和与基底层接触的细胞表面之外。当Na +,K + -ATP酶在18-19 d出现时,与铁蛋白共分布。从成年肠道粘膜上剥离上皮层并没有破坏细胞间连接或侧向细胞接触,但在基底细胞表面出现了胞浆性起泡,并在其中积聚了散布的铁蛋白和肌动蛋白。同时,Na +,K + -ATPase进入基底膜亚结构域,发生了包括Na +,K + -ATPase在内的基底外侧膜的广泛内吞作用。未检测到葡萄膜蛋白的内吞作用,且没有铁蛋白与内吞小泡相关。只要维持细胞间接触,Umormorulin以及一些与膜相关的铁蛋白和一些Na +,K + -ATPase就会保留在外侧膜中。因此,在该极化的上皮中,需要横向细胞-细胞粘附分子的相互作用以及基底细胞-底物的相互作用来维持横向膜骨架的稳定性和在横向膜域中集中的驻留膜蛋白的位置。

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  • 年度 1989
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  • 正文语种 {"code":"en","name":"English","id":9}
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