首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Influence of a reconstituted basement membrane and its components on casein gene expression and secretion in mouse mammary epithelial cells.
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Influence of a reconstituted basement membrane and its components on casein gene expression and secretion in mouse mammary epithelial cells.

机译:重构的基膜及其成分对酪蛋白基因在小鼠乳腺上皮细胞中表达和分泌的影响。

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摘要

When primary mouse mammary epithelial cells are cultured on plastic, they rapidly lose their ability to synthesize and secrete most milk proteins even in the presence of lactogenic hormones, whereas cells cultured on released type I collagen gels show greatly enhanced mRNA levels and secretion rates of beta-casein and of some other milk proteins. We show here that culture on a reconstituted basement membrane from Engelbreth-Holm-Swarm tumor (EHS) allows greater than 90% of cells to produce high levels of beta-casein. By comparison, 30-40% of cells on released type 1 gels and only 2-10% of cells on plastic express beta-casein after 6 days in culture. Because only 40% of cells from late pregnant gland produced beta-casein before culture, the EHS matrix can both induce and maintain an increased level of casein gene expression. Individual basal lamina components were also evaluated. Type IV collagen and fibronectin had little effect on morphology and beta-casein mRNA levels. In contrast, both laminin and heparan sulfate proteoglycan increased beta-casein mRNA levels (1.5- to 4-fold and 2- to 8-fold, respectively). However, for heparan sulfate proteoglycan, increased message was not accompanied by increased secretion of beta-casein. Profound morphological differences were evident between cells cultured on plastic and on EHS matrix, the latter cells forming ducts, ductules, and lumina and resembling secretory alveoli. These results emphasize the vital role of the extracellular matrix in receiving and integrating structural and functional signals that can direct specific gene expression in differentiated tissues.
机译:当小鼠原代乳腺上皮细胞在塑料上培养时,即使存在生乳激素,它们也会迅速失去合成和分泌大多数乳蛋白的能力,而在释放的I型胶原蛋白凝胶上培养的细胞显示出大大提高的mRNA水平和β分泌率-酪蛋白和一些其他牛奶蛋白。我们在这里显示,从Engelbreth-Holm-Swarm肿瘤(EHS)重建的基底膜上进行培养可让90%以上的细胞产生高水平的β-酪蛋白。相比之下,培养6天后,释放的1型凝胶上有30-40%的细胞表达,而塑料上只有2-10%的细胞表达β-酪蛋白。因为只有40%的晚期妊娠腺细胞在培养前产生β-酪蛋白,所以EHS基质既可以诱导也可以维持酪蛋白基因表达水平的提高。还评估了单个基底层成分。 IV型胶原蛋白和纤连蛋白对形态和β-酪蛋白mRNA水平影响很小。相反,层粘连蛋白和硫酸乙酰肝素蛋白聚糖均增加了β-酪蛋白的mRNA水平(分别为1.5至4倍和2至8倍)。然而,对于硫酸乙酰肝素蛋白聚糖,增加的信息并不伴随β-酪蛋白的分泌增加。在塑料和EHS基质上培养的细胞之间存在明显的形态学差异,后一种细胞形成导管,小管和管腔,并类似于分泌性肺泡。这些结果强调了细胞外基质在接收和整合可指导分化组织中特定基因表达的结构和功能信号中的重要作用。

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