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新型MUC1肿瘤抗原亚型在人上皮性肿瘤中的优先表达及其肿瘤促进功能。

Preferential expression of novel MUC1 tumor antigen isoforms in human epithelial tumors and their tumor-potentiating function.

作者信息

Baruch A, Hartmann M, Zrihan-Licht S, Greenstein S, Burstein M, Keydar I, Weiss M, Smorodinsky N, Wreschner D H

机构信息

Department of Cell Research and Immunology, The George S. Wise Faculty of Life Sciences, Tel Aviv University, Ramat Aviv, Israel.

出版信息

Int J Cancer. 1997 May 29;71(5):741-9. doi: 10.1002/(sici)1097-0215(19970529)71:5<741::aid-ijc9>3.0.co;2-r.

Abstract

The human MUC1 gene expresses at least 2 type 1 membrane proteins: MUC1/REP, a polymorphic high m.w. MUC1 glycoprotein often highly expressed in breast cancer tissues and containing a variable number of tandem 20 amino acid repeat units, and the MUC1/Y protein, which lacks this repeat array and, therefore, is not polymorphic. Despite their documented importance in signal transduction processes, the relative expression of the 2 isoforms in epithelial tumors is unknown. Using antibody reagents which recognize different MUC1 domains, the expression of these isoforms in malignant epithelial cells has been evaluated. A comparison of the amounts of the 2 isoforms revealed preferential expression of the novel MUC1/Y protein in breast cancer tissue samples. Furthermore, although the MUC1/REP protein is almost undetectable in HeLa cervical adenocarcinoma epithelial cells, the MUC1/Y isoform is extensively expressed in these cells. The presence of the MUC1/Y sequence as well as that of an additional tandem-repeat-array-lacking isoform, designated MUC1/X, were demonstrated by reverse transcriptase PCR amplification of RNA extracted from HeLa and ovarian carcinoma cells. It has been shown previously that the MUC1 cytoplasmic domain interacts with the SH2 domain containing GRB2 protein, which transduces signals to ras, a protein which in its activated form can lead to cell transformation. We present here data demonstrating that MUC1/Y isoform expression increases the tumorigenic potential of DA3 mouse mammary epithelial cells; in contrast, potentiation of tumorigenicity is not observed with MUC1/REP expression. Our studies thus demonstrate that expression of the MUC1 gene in epithelial tumors can give rise to substantial levels of MUC1 proteins devoid of the tandem repeat array, which are generated by alternative splicing mechanisms.

摘要

人类MUC1基因表达至少两种1型膜蛋白:MUC1/REP,一种多态性高分子量MUC1糖蛋白,常在乳腺癌组织中高表达,含有可变数量的20个氨基酸串联重复单元;以及MUC1/Y蛋白,它缺乏这种重复序列,因此没有多态性。尽管它们在信号转导过程中的重要性已得到证实,但这两种异构体在上皮肿瘤中的相对表达情况尚不清楚。使用识别不同MUC1结构域的抗体试剂,对这些异构体在恶性上皮细胞中的表达进行了评估。两种异构体含量的比较显示,新型MUC1/Y蛋白在乳腺癌组织样本中优先表达。此外,虽然在HeLa宫颈腺癌上皮细胞中几乎检测不到MUC1/REP蛋白,但MUC1/Y异构体在这些细胞中广泛表达。通过对从HeLa细胞和卵巢癌细胞中提取的RNA进行逆转录酶PCR扩增,证实了MUC1/Y序列以及另一种缺乏串联重复序列的异构体MUC1/X的存在。先前已表明,MUC1胞质结构域与含有GRB2蛋白的SH2结构域相互作用,GRB2蛋白将信号转导至ras,ras蛋白的激活形式可导致细胞转化。我们在此展示的数据表明,MUC1/Y异构体的表达增加了DA3小鼠乳腺上皮细胞的致瘤潜力;相比之下,MUC1/REP的表达未观察到致瘤性增强。因此,我们的研究表明,MUC1基因在上皮肿瘤中的表达可产生大量缺乏串联重复序列的MUC1蛋白,这些蛋白是通过可变剪接机制产生的。

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