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α(1,3)-岩藻糖基转移酶基因的表达增强与E-选择素介导的人肺腺癌细胞黏附及转移潜能相关。

Enhanced expression of alpha(1,3)-fucosyltransferase genes correlates with E-selectin-mediated adhesion and metastatic potential of human lung adenocarcinoma cells.

作者信息

Martín-Satué M, Marrugat R, Cancelas J A, Blanco J

机构信息

Departamento Biologia Cellular, Institut de Recerca Oncológia, Barcelona, Spain.

出版信息

Cancer Res. 1998 Apr 1;58(7):1544-50.

PMID:9537262
Abstract

Alpha(1,3)- and alpha(1,4)-fucosylated oligosaccharides such as sialyl-Lewis(x) (sialyl-Le(x)) and sialyl-Lewis(a) (sialyl-Le(a)) have been reported to participate in tumor cell adhesion to activated endothelium. We examined by cytofluorometry the expression of Le(x), sialyl-Le(x), sialyl-Le(x) dimeric, Le(a), and sialyl-Le(a) on the surface of two human lung adenocarcinoma cell lines with different lung colonization potential. High expression levels of all of these antigens were detected in the metastatic HAL-8Luc cells, whereas the closely related nonmetastatic HAL-24Luc cells only expressed the sialyl-Le(a) and sialyl-Le(x) dimeric antigens, both at lower level than in HAL-8Luc cells. Five alpha(1,3)-fucosyltransferases (alpha(1,3)-Fuc-T) controlling the synthesis of these molecules have been identified to date (Fuc-TIII-Fuc-IVII). The expression of these five genes was also higher in the metastatic cells than in the nonmetastatic counterparts as was shown by Northern blot analysis. In vitro adhesion assays showed that only the metastatic cell line adheres significantly to E-selectin-expressing human endothelial cells. Moreover, monoclonal antibody (mAb) blockade of E-selectin completely abolished tumor cell binding. Adhesion inhibition experiments using mAbs against sialylated fucosylated oligosaccharides expressed on tumor cells indicated that these antigens are involved in the binding. Anti-sialyl-Lex(x) mAb (CSLEX-1) inhibited adhesion by 85%; it had the most pronounced inhibitory effect. These findings suggest that the overexpression of alpha(1,3)-Fuc-T genes in the metastatic HAL-8Luc cells, compared with HAL-24Luc cells, results in an enhanced surface display of fucosylated oligosaccharides, which contributes to the adhesive capacity of these cells to the activated endothelium and correlates with their lung colonization potential.

摘要

据报道,α(1,3)-和α(1,4)-岩藻糖基化寡糖,如唾液酸化路易斯(x)(唾液酸化Le(x))和唾液酸化路易斯(a)(唾液酸化Le(a))参与肿瘤细胞与活化内皮细胞的黏附。我们通过细胞荧光术检测了两种具有不同肺定植潜能的人肺腺癌细胞系表面Le(x)、唾液酸化Le(x)、唾液酸化Le(x)二聚体、Le(a)和唾液酸化Le(a)的表达。在转移性HAL-8Luc细胞中检测到所有这些抗原的高表达水平,而密切相关的非转移性HAL-24Luc细胞仅表达唾液酸化Le(a)和唾液酸化Le(x)二聚体抗原,且两者表达水平均低于HAL-8Luc细胞。迄今为止,已鉴定出5种控制这些分子合成的α(1,3)-岩藻糖基转移酶(α(1,3)-Fuc-T)(Fuc-TIII - Fuc-IVII)。如Northern印迹分析所示,这5个基因在转移性细胞中的表达也高于非转移性细胞。体外黏附试验表明,只有转移性细胞系能显著黏附于表达E-选择素的人内皮细胞。此外,E-选择素的单克隆抗体(mAb)阻断完全消除了肿瘤细胞的结合。使用针对肿瘤细胞表面表达的唾液酸化岩藻糖基化寡糖的mAb进行的黏附抑制实验表明,这些抗原参与了结合。抗唾液酸化Lex(x) mAb(CSLEX-1)抑制黏附达85%;其抑制作用最为显著。这些发现表明,与HAL-24Luc细胞相比,转移性HAL-8Luc细胞中α(1,3)-Fuc-T基因的过表达导致岩藻糖基化寡糖在表面的展示增强,这有助于这些细胞对活化内皮细胞的黏附能力,并与其肺定植潜能相关。

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