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“简单”上皮细胞中存在显著的可溶性角蛋白组分。角蛋白溶解性中缺乏明显的磷酸化和糖基化作用。

A significant soluble keratin fraction in 'simple' epithelial cells. Lack of an apparent phosphorylation and glycosylation role in keratin solubility.

作者信息

Chou C F, Riopel C L, Rott L S, Omary M B

机构信息

Palo Alto Veterans Administration Medical Center, CA.

出版信息

J Cell Sci. 1993 Jun;105 ( Pt 2):433-44. doi: 10.1242/jcs.105.2.433.

Abstract

We studied the solubility of keratin polypeptides 8 and 18 (K8/18), which are the predominant intermediate filaments in the human colonic epithelial cell line HT29. We find that asynchronously growing cells (G0/G1 stage of the cell cycle) have a substantial pool of soluble keratin that constitutes approx. 5% of total cellular keratin. This soluble keratin pool was observed after immunoprecipitation of K8/18 from the cytosolic fraction of cells disrupted using three detergent-free methods. Several other cell lines showed a similar significant soluble cytosolic K8/18 pool. Arrest of HT29 cells in G2/M stage of the cell cycle was associated with a concurrent increase in keratin solubility. Comparison of K8/18 obtained from the soluble cytosolic fraction and the insoluble high-speed pellet fraction showed similar levels of phosphorylation and glycosylation and similar tryptic radiolabeled phospho- and glycopeptide patterns. Soluble K8/18 can form characteristic 10 nm filaments in vitro as determined by electron microscopy. Cross-linking of soluble K8/18 followed by immunoprecipitation resulted in dimeric and tetrameric forms, based on migration in SDS-polyacrylamide gels. In addition, cross-linked and native soluble K8/18 showed similar migration on nondenaturing gels and similar sedimentation after sucrose density gradient centrifugation. Our results indicate that simple epithelial keratins are appreciably more soluble than previously recognized. The soluble keratin form is assembly competent and appears to be primarily tetrameric. Although K8/18 solubility was found to increase during mitotic arrest, glycosylation and phosphorylation did not play an obvious role in generating the soluble fraction, suggesting an alternate mechanism for keratin solubility.

摘要

我们研究了角蛋白多肽8和18(K8/18)的溶解性,它们是人类结肠上皮细胞系HT29中主要的中间丝。我们发现,处于细胞周期G0/G1期的异步生长细胞有大量可溶性角蛋白池,约占细胞总角蛋白的5%。在用三种无去污剂方法破坏细胞的胞质部分后,通过免疫沉淀K8/18观察到了这个可溶性角蛋白池。其他几种细胞系也显示出类似的显著可溶性胞质K8/18池。HT29细胞在细胞周期G2/M期的停滞与角蛋白溶解性的同时增加有关。从可溶性胞质部分和不溶性高速沉淀部分获得的K8/18的磷酸化和糖基化水平相似,胰蛋白酶放射性标记的磷酸肽和糖肽模式也相似。通过电子显微镜测定,可溶性K8/18在体外可形成特征性的10纳米细丝。基于在SDS-聚丙烯酰胺凝胶中的迁移,可溶性K8/18交联后再进行免疫沉淀会产生二聚体和四聚体形式。此外,交联的和天然的可溶性K8/18在非变性凝胶上显示出相似的迁移,在蔗糖密度梯度离心后沉降情况也相似。我们的结果表明,简单上皮角蛋白的溶解性比以前认为的要明显更高。可溶性角蛋白形式具有组装能力,似乎主要是四聚体。虽然发现K8/18的溶解性在有丝分裂停滞期间增加,但糖基化和磷酸化在产生可溶性部分中并未发挥明显作用,这表明角蛋白溶解性存在另一种机制。

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