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针对不同 Tn-氨基酸骨架的单克隆抗体在人类癌细胞上显示出不同的识别模式。对癌症有效免疫靶向的影响。

Monoclonal antibodies toward different Tn-amino acid backbones display distinct recognition patterns on human cancer cells. Implications for effective immuno-targeting of cancer.

机构信息

Departamento de Anatomía Patológica y Citología del Hospital de la Mujer, Centro Hospitalario Pereira Rossell, Montevideo, Uruguay.

出版信息

Cancer Immunol Immunother. 2013 Jun;62(6):1107-22. doi: 10.1007/s00262-013-1425-7. Epub 2013 Apr 21.

Abstract

The Tn antigen (GalNAcα-O-Ser/Thr) is a well-established tumor-associated marker which represents a good target for the design of anti-tumor vaccines. Several studies have established that the binding of some anti-Tn antibodies could be affected by the density of Tn determinant or/and by the amino acid residues neighboring O-glycosylation sites. In the present study, using synthetic Tn-based vaccines, we have generated a panel of anti-Tn monoclonal antibodies. Analysis of their binding to various synthetic glycopeptides, modifying the amino acid carrier of the GalNAc() (Ser vs Thr*), showed subtle differences in their fine specificities. We found that the recognition of these glycopeptides by some of these MAbs was strongly affected by the Tn backbone, such as a SSS* specific MAb (15G9) which failed to recognize a STT* or a TTT* structure. Different binding patterns of these antibodies were also observed in FACS and Western blot analysis using three human cancer cell lines (MCF-7, LS174T and Jurkat). Importantly, an immunohistochemical analysis of human tumors (72 breast cancer and 44 colon cancer) showed the existence of different recognition profiles among the five antibodies evaluated, demonstrating that the aglyconic part of the Tn structure (Ser vs Thr) plays a key role in the anti-Tn specificity for breast and colon cancer detection. This new structural feature of the Tn antigen could be of important clinical value, notably due to the increasing interest of this antigen in anticancer vaccine design as well as for the development of anti-Tn antibodies for in vivo diagnostic and therapeutic strategies.

摘要

Tn 抗原(GalNAcα-O-Ser/Thr)是一种成熟的肿瘤相关标志物,是设计抗肿瘤疫苗的良好靶标。多项研究已经证实,一些抗-Tn 抗体的结合可能受到 Tn 决定簇的密度和/或邻近 O-糖基化位点的氨基酸残基的影响。在本研究中,我们使用合成的 Tn 疫苗,产生了一组抗-Tn 单克隆抗体。分析它们与各种合成糖肽的结合情况,改变 GalNAc()(Ser 与 Thr*)的氨基酸载体,发现它们的精细特异性存在细微差异。我们发现,这些 MAbs 对这些糖肽的识别受到 Tn 骨架的强烈影响,例如,一种特异性识别 SSS的 MAb(15G9)无法识别 STT或 TTT*结构。在使用三种人类癌细胞系(MCF-7、LS174T 和 Jurkat)的 FACS 和 Western blot 分析中,也观察到这些抗体的不同结合模式。重要的是,对 72 例乳腺癌和 44 例结肠癌患者肿瘤的免疫组织化学分析显示,在所评估的 5 种抗体中存在不同的识别谱,表明 Tn 结构的糖苷部分(Ser 与 Thr)在乳腺癌和结肠癌检测的抗-Tn 特异性中起关键作用。这种 Tn 抗原的新结构特征可能具有重要的临床价值,特别是由于该抗原在抗癌疫苗设计中的重要性不断增加,以及用于体内诊断和治疗策略的抗-Tn 抗体的开发。

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