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A newly generated functional antibody identifies Tn antigen as a novel determinant in the cancer cell–lymphatic endothelium interaction

机译:一种新产生的功能性抗体将Tn抗原鉴定为癌细胞与淋巴管内皮相互作用的新决定因素

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摘要

Malignant transformation of epithelial cells is frequently associated with the alteration of glycosylation pathways. Tn is a common tumor-associated carbohydrate antigen present in 90% of human carcinomas and its expression correlates with metastatic potential and poor prognosis. Despite its relevance, the functional role of Tn in tumor biology has not been firmly established probably for the lack of appropriate experimental tools. Our aims were to produce highly reactive monoclonal antibodies against Tn making use of synthetically produced Tn and to test their usefulness for in vivo imaging as well as to define their potential functional activity in tumor cell spread. We immunized mice with Tn clustered on cationized BSA and screened the positive hybridomas with Tn-biotinylated alginate. Enzyme-linked immuno sorbent assay and immunofluorescence assays revealed that the most reactive anti-Tn IgM mAb (2154F12A4) selectively recognized Tn on the MCF7 breast cancer cell line since its binding to the cell membrane was completely abolished by preincubation with purified Tn. Importantly, QDot 800-conjugated mAb injected in MCF7-tumor bearing mice specifically bound to primary tumor lesions as well as to metastases in lymph nodes. In addition, this mAb was able to inhibit cancer cell adhesion to lymphatic endothelium suggesting a novel involvement of Tn in the lymphatic dissemination of cancer cells and hypothesizing future applications in inhibiting lymphatic metastases.
机译:上皮细胞的恶性转化通常与糖基化途径的改变有关。 Tn是90%的人类癌症中常见的与肿瘤相关的糖类抗原,其表达与转移潜能和预后不良相关。尽管具有相关性,但由于缺乏合适的实验工具,Tn在肿瘤生物学中的功能尚未得到牢固确立。我们的目标是利用合成产生的Tn产生针对Tn的高反应性单克隆抗体,并测试其在体内成像中的作用以及定义其在肿瘤细胞扩散中的潜在功能活性。我们用在阳离子化BSA上聚集的Tn免疫小鼠,并用Tn生物素化藻酸盐筛选阳性杂交瘤。酶联免疫吸附测定和免疫荧光测定显示,最具反应性的抗Tn IgM mAb(2154F12A4)选择性识别MCF7乳腺癌细胞系上的Tn,因为通过与纯化Tn的预孵育而完全消除了其与细胞膜的结合。重要的是,在携带MCF7肿瘤的小鼠中注射QDot 800偶联的mAb特异性结合原发性肿瘤病变以及淋巴结转移。另外,该mAb能够抑制癌细胞与淋巴内皮的粘附,这表明Tn参与了癌细胞的淋巴扩散,并推测了其在抑制淋巴转移中的未来应用。

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