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肿瘤细胞MUC1和CD43在唾液酸化刘易斯a和x表位上的糖基化方式不同,并且在生理流动条件下与E-选择素表现出不同的相互作用。

Tumor cell MUC1 and CD43 are glycosylated differently with sialyl-Lewis a and x epitopes and show variable interactions with E-selectin under physiological flow conditions.

作者信息

Fernandez-Rodriguez J, Dwir O, Alon R, Hansson G C

机构信息

Department of Medical Biochemistry, Göteborg University, Box 440, 405 30 Gothenburg, Sweden.

出版信息

Glycoconj J. 2001 Nov-Dec;18(11-12):925-30. doi: 10.1023/a:1022208727512.

Abstract

The mucins secreted from the colon carcinoma cell line COLO 205 have the MUC1 and CD43 (leukosialin) as core proteins, where both carry sialyl-Lewis a and MUC1 sialyl-Lewis x epitopes. The adhesion of E-selectin expressing CHO cells to the coated mucins was analyzed in a flow system revealing that the MUC1 mucin adhered better than the CD43 mucin. One reason could be their different glycosylation, a difference that was explored by analyzing the biosynthesis of MUC1 and CD43 in COLO 205 cells. Both the MUC1 and CD43 mucins became sialyl-Lewis a reactive, but after different times as revealed by pulse-chase studies. However, only MUC1 became sialyl-Lewis x reactive. These differences suggest that MUC1 and CD43 are synthesized in different compartments of the cell. It was also observed that the mucins from colon carcinoma patients had MUC1-type mucins that carried both sialyl-Lewis a and x epitopes and CD43-type sialyl-Lewis a mucins with only low levels of sialyl-Lewis x epitopes. One could hypothesize that colon carcinoma derived MUC1 is decorated with potent E-selectin epitopes, and that this could be one of several reasons for the involvement of MUC1 in cancer development.

摘要

结肠癌细胞系COLO 205分泌的黏蛋白以MUC1和CD43(白细胞涎酸蛋白)作为核心蛋白,二者均携带唾液酸化路易斯a以及MUC1唾液酸化路易斯x表位。在流动系统中分析表达E-选择素的CHO细胞与包被的黏蛋白之间的黏附情况,结果显示MUC1黏蛋白比CD43黏蛋白的黏附性更好。原因之一可能是它们的糖基化不同,通过分析COLO 205细胞中MUC1和CD43的生物合成来探究这种差异。脉冲追踪研究显示,MUC1和CD43黏蛋白均具有唾液酸化路易斯a反应性,但时间不同。然而,只有MUC1具有唾液酸化路易斯x反应性。这些差异表明MUC1和CD43在细胞的不同区室中合成。还观察到结肠癌患者的黏蛋白中有携带唾液酸化路易斯a和x表位的MUC1型黏蛋白以及唾液酸化路易斯x表位水平较低的CD43型唾液酸化路易斯a黏蛋白。可以推测,结肠癌来源的MUC1带有有效的E-选择素表位,这可能是MUC1参与癌症发展的几个原因之一。

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