首页> 外文OA文献 >Appearance in confluent vascular endothelial cell monolayers of a specific cell surface protein (CSP-60) not detected in actively growing endothelial cells or in cell types growing in multiple layers.
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Appearance in confluent vascular endothelial cell monolayers of a specific cell surface protein (CSP-60) not detected in actively growing endothelial cells or in cell types growing in multiple layers.

机译:在活跃生长的内皮细胞或多层生长的细胞类型中未检测到特定细胞表面蛋白(CSP-60)的融合血管内皮细胞单层的外观。

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摘要

The formation of a highly organized vascular and corneal endothelial cell monolayer is associated with the appearance of a 60,000-dalton cell surface protein (CSP-60) (30,000 daltons after reduction with dithiothreitol) which is not detectable in rapidly growing endothelial cells and in subconfluent cultures that do not yet exhibit the strict morphology of a confluent monolayer. It is also absent from vascular smooth muscle cells and from endothelial cultures that are maintained in the absence of fibroblast growth factor and grow on top of each other at confluence. After disorganization of cells in a confluent endothelial monolayer by urea, EDTA, or trypsin, CPS-60 is no longer exposed on the cell surface, but it reappears as soon as the cells readopt their characteristic two-dimensional configuration. This reorganization can be achieved in the presence of cycloheximide and despite removal of fibronectin by urea, EDTA, or trypsin. Maximal amounts of fibronectin and no CSP-60 are detected in subconfluent, but not yet organized, endothelial cultures or in endothelial cells that no longer form a monolayer of nonoverlapping cells at confluence. Likewise, cultures of vascular smooth muscle cells contain fibronectin but no CSP-60. These results suggest that CSP-60, rather than fibronectin, could be involved in the adoption of a monolayer configuration by confluent endothelial cells.
机译:高度组织化的血管和角膜内皮细胞单层的形成与60,000道尔顿的细胞表面蛋白(CSP-60)(用二硫苏糖醇还原后的30,000道尔顿)的出现有关,在快速生长的内皮细胞和亚汇合中无法检测到尚未显示出融合单层的严格形态的细菌培养物。在缺乏成纤维细胞生长因子的情况下维持的血管平滑肌细胞和内皮培养物中也缺乏这种蛋白,它们在汇合处彼此重叠生长。在通过尿素,EDTA或胰蛋白酶使汇合的内皮单层细胞解体后,CPS-60不再暴露于细胞表面,但只要细胞重新采用其特征性的二维结构,它就会重新出现。在存在环己酰亚胺的情况下,尽管通过尿素,EDTA或胰蛋白酶去除了纤连蛋白,也可以实现这种重组。在亚融合但尚未组织的内皮培养物中或在融合时不再形成单层非重叠细胞的内皮细胞中,检测到最大量的纤连蛋白且未检测到CSP-60。同样,血管平滑肌细胞培养物中含有纤连蛋白,但不含CSP-60。这些结果表明,CSP-60,而不是纤连蛋白,可能参与了融合内皮细胞采用单层构型。

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