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Selectin Ligands Sialyl-Lewis a and Sialyl-Lewis x in Gastrointestinal Cancers

机译:Selectin配体在胃肠道癌症中的唾液酸化-刘易斯a和唾液酸化-刘易斯x

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摘要

The tetrasaccharide structures Siaα2,3Galβ1,3(Fucα1,4)GlcNAc and Siaα2,3Galβ1,4(Fucα1,3)GlcNAc constitute the epitopes of the carbohydrate antigens sialyl-Lewis a (sLea) and sialyl-Lewis x (sLex), respectively, and are the minimal requirement for selectin binding to their counter-receptors. Interaction of sLex expressed on the cell surface of leucocytes with E-selectin on endothelial cells allows their arrest and promotes their extravasation. Similarly, the rolling of cancer cells ectopically expressing the selectin ligands on endothelial cells is potentially a crucial step favoring the metastatic process. In this review, we focus on the biosynthetic steps giving rise to selectin ligand expression in cell lines and native tissues of gastrointestinal origin, trying to understand whether and how they are deregulated in cancer. We also discuss the use of such molecules in the diagnosis of gastrointestinal cancers, particularly in light of recent data questioning the ability of colon cancers to express sLea and the possible use of circulating sLex in the early detection of pancreatic cancer. Finally, we reviewed the data dealing with the mechanisms that link selectin ligand expression in gastrointestinal cells to cancer malignancy. This promising research field seems to require additional data on native patient tissues to reach more definitive conclusions.
机译:四糖结构Siaα2,3Galβ1,3(Fucα1,4)GlcNAc和Siaα2,3Galβ1,4(Fucα1,3)GlcNAc构成碳水化合物抗原sialyl-Lewis a(sLe a )和sialyl的表位-Lewis x(sLe x ),分别是selectin与其反受体结合的最低要求。在白细胞的细胞表面表达的sLe x 与内皮细胞上的E-选择素相互作用,可使其停滞并促进其外渗。同样,在内皮细胞上异位表达选择蛋白配体的癌细胞的滚动可能是促进转移过程的关键步骤。在这篇综述中,我们集中于引起胃肠道起源的细胞系和天然组织中选择素配体表达的生物合成步骤,试图了解它们是否以及如何在癌症中被失调。我们还将讨论这种分子在胃肠道癌诊断中的用途,尤其是根据最近的数据质疑结肠癌表达sLe a 的能力以及循环使用的sLe x < / sup>在胰腺癌的早期发现中。最后,我们回顾了有关胃肠道细胞中选择素配体表达与癌症恶性联系的机制的数据。这个有前途的研究领域似乎需要更多有关天然患者组织的数据才能得出更明确的结论。

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