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人类结肠癌细胞的肝转移及对窦状内皮的黏附与黏蛋白碳水化合物链长度有关。

Liver metastasis and adhesion to the sinusoidal endothelium by human colon cancer cells is related to mucin carbohydrate chain length.

作者信息

Bresalier R S, Byrd J C, Brodt P, Ogata S, Itzkowitz S H, Yunker C K

机构信息

Department of Medicine, Henry Ford Health Sciences Center, Detroit, MI 48202, USA.

出版信息

Int J Cancer. 1998 May 18;76(4):556-62. doi: 10.1002/(sici)1097-0215(19980518)76:4<556::aid-ijc19>3.0.co;2-5.

Abstract

Mucin production by human colon cancer cells correlates with liver metastasis in animal models, but it is not known which steps in metastasis depend on specific alterations in mucin synthesis. Clonal variants of cell line LS174T selected for differences in mucin core carbohydrate expression have been further characterized biochemically, and tested for their ability to participate in metastasis-related events. LS-C mucin contains truncated carbohydrates enriched for sialyl Tn and these cells bind to basement membrane matrix to a greater extent than LS-B cells. This binding is partially inhibitable by antibody to sialyl Tn. LS-B produces more fully glycosylated mucin and preferentially binds to hepatic sinusoidal endothelial cells and E-selectin through sialylated peripheral mucin-associated carbohydrate structures. Adhesion of LS-B to endothelial cells is inhibited by neutralizing antibody to E-selectin, and inhibition of glycosylation or desialylation of LS-B mucin abrogates binding to E-selectin in vitro. LS-B cells spontaneously metastasized from cecum to liver and colonized the liver of athymic mice after splenic-portal injection to a significantly greater extent than LS-C, suggesting that expression of peripheral mucin carbohydrate structures is most important for metastasis of human colon cancer cells.

摘要

在动物模型中,人类结肠癌细胞产生的黏蛋白与肝转移相关,但尚不清楚转移过程中的哪些步骤依赖于黏蛋白合成的特定改变。已对因黏蛋白核心碳水化合物表达差异而筛选出的细胞系LS174T的克隆变体进行了进一步的生化特征分析,并测试了它们参与转移相关事件的能力。LS-C黏蛋白含有富含唾液酸化Tn的截短碳水化合物,这些细胞与基底膜基质的结合程度比LS-B细胞更高。这种结合可被抗唾液酸化Tn抗体部分抑制。LS-B产生的黏蛋白糖基化更完全,并通过唾液酸化的外周黏蛋白相关碳水化合物结构优先与肝窦内皮细胞和E-选择素结合。抗E-选择素的中和抗体可抑制LS-B与内皮细胞的黏附,体外抑制LS-B黏蛋白的糖基化或去唾液酸化可消除其与E-选择素的结合。脾门静脉注射后,LS-B细胞从盲肠自发转移至肝脏并在无胸腺小鼠的肝脏中定植,其程度明显高于LS-C,这表明外周黏蛋白碳水化合物结构的表达对人类结肠癌细胞的转移最为重要。

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