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异常的Cosmc基因导致人结肠癌细胞系HT-29中Tn抗原表达。

Aberrant Cosmc genes result in Tn antigen expression in human colorectal carcinoma cell line HT-29.

作者信息

Yu Xiaofeng, Du Zhenzhen, Sun Xuhong, Shi Chuanqin, Zhang Huaixiang, Hu Tao

机构信息

Department of Immunology, Binzhou Medical University Yantai 264003, P.R. China.

Department of Essentials of Basic Medicine, Binzhou Medical University Yantai, P.R. China.

出版信息

Int J Clin Exp Pathol. 2015 Mar 1;8(3):2590-602. eCollection 2015.

PMID:26045765
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4440074/
Abstract

The Tn antigen, which arises from mutation in the Cosmc gene is one of the most common tumor associated carbohydrate antigens. Cosmc resides in X24 encoded by a single gene and functions as a specific molecular chaperone for T-synthase. While the Tn antigen cannot be detected in normal cells, Cosmc mutations inactivate T-synthase and consequently result in Tn antigen expression within certain cancers. In addition to this Cosmc mutation-induced expression, the Tn antigen is also expressed in such cell lines as Jurkat T, LSC and LS174T. Whether the Cosmc mutation is present in the colon cancer cell line HT-29 is still unclear. Here, we isolate HT-29-Tn+ cells from HT-29 cells derived from a female colon cancer patient. These HT-29-Tn+ cells show a loss of the Cosmc gene coding sequence (CDS) leading to an absence of T-synthase activity and Tn antigen expression. Additionally, almost no methylation of Cosmc CpG islands was detected in HT-29-Tn+ as well as in HT-29-Tn- and Tn- tumor cells from male patients. In contrast, the methylation frequency of CpG island of Cosmc in normal female cells was ~50%. Only one active allele of Cosmc existed in HT-29-Tn+ and HT-29-Tn- cells as based upon detection of SNP sites. These results indicate that Tn antigens expression and T-synthase inactivity in HT-29-Tn+ cells can be related to the absence of CDS in Cosmc active alleles, while an inactive allele deletion of Cosmc in HT-29 cells has no influence on Cosmc function.

摘要

Tn抗原是最常见的肿瘤相关碳水化合物抗原之一,它由Cosmc基因突变产生。Cosmc位于由单基因编码的X24中,作为T合酶的特异性分子伴侣发挥作用。虽然在正常细胞中检测不到Tn抗原,但Cosmc突变会使T合酶失活,从而导致某些癌症中Tn抗原的表达。除了这种由Cosmc突变诱导的表达外,Tn抗原也在Jurkat T、LSC和LS174T等细胞系中表达。结肠癌细胞系HT-29中是否存在Cosmc突变仍不清楚。在这里,我们从一名女性结肠癌患者的HT-29细胞中分离出HT-29-Tn+细胞。这些HT-29-Tn+细胞显示Cosmc基因编码序列(CDS)缺失,导致T合酶活性缺失和Tn抗原表达缺失。此外,在HT-29-Tn+以及来自男性患者 的HT-29-Tn-和Tn-肿瘤细胞中几乎未检测到Cosmc CpG岛的甲基化。相比之下,正常女性细胞中Cosmc CpG岛的甲基化频率约为50%。基于SNP位点的检测,HT-29-Tn+和HT-29-Tn-细胞中仅存在一个Cosmc活性等位基因。这些结果表明,HT-29-Tn+细胞中Tn抗原的表达和T合酶的无活性可能与Cosmc活性等位基因中CDS的缺失有关,而HT-29细胞中Cosmc的无活性等位基因缺失对Cosmc功能没有影响。

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