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首页> 外文期刊>Journal of cell biology >A specific sorting signal is not required for the polarized secretion of newly synthesized proteins from cultured intestinal epithelial cells.
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A specific sorting signal is not required for the polarized secretion of newly synthesized proteins from cultured intestinal epithelial cells.

机译:从培养的肠上皮细胞极化分泌新合成的蛋白质不需要特定的分类信号。

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摘要

Caco-2 cells, derived from human colon, have the morphological, functional, and biochemical properties of small intestinal epithelial cells. After infection with enveloped viruses, influenza virions assembled at the apical plasma membrane while vesicular stomatitis virus (VSV) particles appeared exclusively at the basolateral membrane, similar to the pattern observed in virus-infected Madin-Darby canine kidney (MDCK). When grown in Millicell filter chamber devices and labeled with [35S]methionine, Caco-2 monolayers released all of their radiolabeled secretory products preferentially into the basal chamber. Among the proteins identified were apolipoproteins AI and E, transferrin, and alpha-fetoprotein. No proteins were observed to be secreted preferentially from the apical cell surface. The lysosomal enzyme beta-hexosaminidase was also secreted primarily from the basolateral surface of the cells in the presence or absence of lysosomotropic drugs or tunicamycin, which inhibit the targetting of lysosomal enzymes to lysosomes. Neither of these drug treatments significantly affected the polarized secretion of other nonlysosomal proteins. In addition, growth hormone (GH), which is released in a nonpolar fashion from MDCK cells, was secreted exclusively from the basolateral membrane after transfection of Caco-2 cells with GH cDNA in a pSV2-based expression vector. Similar results were obtained in transient expression experiments and after selection of permanently transformed Caco-2 cells expressing GH. Since both beta-hexosaminidase and GH would be expected to lack sorting signals for polarized exocytosis in epithelial cells, these results indicate that in intestinal cells, proteins transported via the basolateral secretory pathway need not have specific sorting signals.
机译:源自人类结肠的Caco-2细胞具有小肠上皮细胞的形态,功能和生化特性。在被包膜病毒感染后,流感病毒颗粒聚集在顶质膜上,而水泡性口炎病毒(VSV)颗粒仅出现在基底外侧膜上,类似于在病毒感染的Madin-Darby犬肾(MDCK)中观察到的模式。当在Millicell过滤室设备中生长并用[35S]蛋氨酸标记时,Caco-2单分子膜将所有放射性标记的分泌产物优先释放到基室中。在鉴定出的蛋白质中,载脂蛋白AI和E,转铁蛋白和甲胎蛋白。没有观察到蛋白质优先从顶端细胞表面分泌。在存在或不存在溶酶体药物或衣霉素的情况下,溶酶体酶β-己糖胺酶也主要从细胞的基底外侧表面分泌,这抑制了溶酶体酶靶向溶酶体。这些药物治疗均未显着影响其他非溶酶体蛋白的极化分泌。此外,在基于pSV2的表达载体中,用GH cDNA转染Caco-2细胞后,以非极性方式从MDCK细胞中释放的生长激素(GH)仅从基底外侧膜分泌。在瞬时表达实验中以及选择表达GH的永久转化的Caco-2细胞后,获得了相似的结果。由于预计β-己糖胺酶和GH都缺乏上皮细胞极化胞吐作用的分类信号,因此这些结果表明,在肠道细胞中,通过基底外侧分泌途径转运的蛋白质不需要具有特定的分类信号。

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