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细胞表面蛋白聚糖在小鼠乳腺上皮细胞的基底外侧细胞表面与细胞骨架结合。

Cell surface proteoglycan associates with the cytoskeleton at the basolateral cell surface of mouse mammary epithelial cells.

作者信息

Rapraeger A, Jalkanen M, Bernfield M

出版信息

J Cell Biol. 1986 Dec;103(6 Pt 2):2683-96. doi: 10.1083/jcb.103.6.2683.

Abstract

The cell surface proteoglycan on normal murine mammary gland mouse mammary epithelial cells consists of an ectodomain bearing heparan and chondroitin sulfate chains and a lipophilic domain that is presumed to be intercalated into the plasma membrane. Because the ectodomain binds to matrix components produced by stromal cells with specificity and high affinity, we have proposed that the cell surface proteoglycan is a matrix receptor that binds epithelial cells to their underlying basement membrane. We now show that the proteoglycan surrounds cells grown in subconfluent or newly confluent monolayers, but becomes restricted to the basolateral surface of cells that have been confluent for a week or more; Triton X-100 extraction distinguishes three fractions of cell surface proteoglycan: a fraction released by detergent and presumed to be free in the membrane, a fraction bound via a salt-labile linkage, and a nonextractable fraction; the latter two fractions co-localize with actin filament bundles at the basal cell surface; and when proteoglycans at the apical cell surface are cross-linked by antibodies, they initially assimilate into detergent-resistant, immobile clusters that are subsequently aggregated by the cytoskeleton. These findings suggest that the proteoglycan, initially present on the entire surface and free in the plane of the membrane, becomes sequestered at the basolateral cell surface and bound to the actin-rich cytoskeleton as the cells become polarized in vitro. Binding of matrix components may cross-link proteoglycans at the basal cell surface and cause them to associate with the actin cytoskeleton, providing a mechanism by which the cell surface proteoglycan acts as a matrix receptor to stabilize the morphology of epithelial sheets.

摘要

正常小鼠乳腺上皮细胞表面的蛋白聚糖由一个带有硫酸乙酰肝素和硫酸软骨素链的胞外结构域以及一个被认为插入质膜的亲脂结构域组成。由于胞外结构域能特异性且高亲和力地结合基质细胞产生的基质成分,我们提出细胞表面蛋白聚糖是一种将上皮细胞与其下方基底膜结合的基质受体。我们现在发现,蛋白聚糖围绕着以亚汇合或新汇合单层生长的细胞,但在汇合一周或更长时间的细胞中,它会局限于细胞的基底外侧表面;Triton X-100提取法可区分细胞表面蛋白聚糖的三个部分:一部分由去污剂释放,推测在膜中是游离的;一部分通过对盐不稳定的连接键结合;还有一部分是不可提取的部分;后两部分在基底细胞表面与肌动蛋白丝束共定位;当顶端细胞表面的蛋白聚糖被抗体交联时,它们最初会聚集到抗去污剂的、不动的簇中,随后这些簇会被细胞骨架聚集起来。这些发现表明,最初存在于整个表面且在膜平面内游离的蛋白聚糖,在细胞体外极化时会被隔离在基底外侧细胞表面,并与富含肌动蛋白的细胞骨架结合。基质成分的结合可能会在基底细胞表面交联蛋白聚糖,并使其与肌动蛋白细胞骨架结合,从而提供一种机制,通过这种机制细胞表面蛋白聚糖作为基质受体来稳定上皮细胞片层的形态。

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