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卵巢癌细胞与固定化透明质酸的结合。

Binding of ovarian cancer cells to immobilized hyaluronic acid.

作者信息

Catterall J B, Gardner M J, Jones L M, Turner G A

机构信息

Department of Clinical Biochemistry, Medical School, Framlington Place, Newcastle upon Tyne, UK.

出版信息

Glycoconj J. 1997 Aug;14(5):647-9. doi: 10.1023/a:1018500929514.

Abstract

Ovarian cancer has the highest mortality rate of any gynaecological malignancy. This is caused by metastatic deposits obstructing the intestinal tract. Very little is known about the molecules involved in the initial attachment of the metastatic tumour cells to the peritoneal mesothelial lining. Previously, we showed that many ovarian tumour lines express the adhesion molecule, CD44, on their cell surface. The major ligand for CD44 is the extracellular matrix glycosaminoglycan, hyaluronic acid (HA). Because mesothelial cells have a pericellular cost that contains large amounts of HA, it was postulated that the CD44/HA interaction is an important stage in ovarian cancer spread. However, it was difficult to demonstrate this interaction in an in vitro adhesion assay with mesothelial cells as most of the HA, and presumably the bound tumour cells, were lost from the mesothelial cells during the washing steps of the assay. In order to try and clarify the situation, the adhesion of six ovarian tumour lines to immobilized HA was measured. Four lines expressed high levels of CD44 and two lines expressed negligible amounts. Preliminary experiments were carried out with one of the CD44-expressing lines. After coating a plate overnight with 3 mg ml(-1) HA, the 5 min adhesion of this line varied between 2% and 73% according to the type of plate that was used. Falcon Micro Test III flexible plates gave the highest adhesion and was used for further experiments. Plates were coated with concentrations of HA between 0.001 mg ml(-1) and 3 mg ml(-1). All CD44 expressing lines adhered to HA, but the maximum adhesion and the adhesion strength varied with the line studied and was not closely related to the total CD44 expression. These results suggest that CD44 on ovarian tumour cells binds to HA on mesothelial cells. As much of the HA can be very easily lost from the mesothelial cell surface, additional factors such as the strength of the CD44/HA interaction, and the formation of bonds by the tumour cells with other membrane adhesion molecules, such as integrins, are also important in promoting tumour spread.

摘要

卵巢癌是所有妇科恶性肿瘤中死亡率最高的。这是由转移瘤阻塞肠道所致。对于转移性肿瘤细胞最初附着于腹膜间皮衬里所涉及的分子,人们了解甚少。此前,我们发现许多卵巢肿瘤细胞系在其细胞表面表达黏附分子CD44。CD44的主要配体是细胞外基质糖胺聚糖透明质酸(HA)。由于间皮细胞有一个富含大量HA的细胞周基质,因此推测CD44/HA相互作用是卵巢癌扩散的一个重要阶段。然而,在与间皮细胞进行的体外黏附试验中,很难证明这种相互作用,因为在试验的洗涤步骤中,大部分HA以及可能与之结合的肿瘤细胞都从间皮细胞上丢失了。为了试图澄清这种情况,我们检测了6种卵巢肿瘤细胞系对固定化HA的黏附情况。其中4种细胞系表达高水平的CD44,2种细胞系表达量可忽略不计。我们用其中一种表达CD44的细胞系进行了初步实验。用3 mg/ml的HA在平板上包被过夜后,根据所用平板的类型,该细胞系5分钟的黏附率在2%至73%之间变化。Falcon Micro Test III柔性平板的黏附率最高,并用于进一步实验。平板用浓度在0.001 mg/ml至3 mg/ml之间的HA包被。所有表达CD44的细胞系都能黏附于HA,但最大黏附率和黏附强度因所研究的细胞系而异,且与总的CD44表达量没有密切关系。这些结果表明,卵巢肿瘤细胞上的CD44与间皮细胞上的HA结合。由于许多HA很容易从间皮细胞表面丢失,其他因素,如CD44/HA相互作用的强度,以及肿瘤细胞与其他膜黏附分子(如整合素)形成的键,在促进肿瘤扩散中也很重要。

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