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人全长 MUC1 的表达抑制 B16 小鼠黑色素瘤细胞系的增殖和迁移。

Expression of human full-length MUC1 inhibits the proliferation and migration of a B16 mouse melanoma cell line.

机构信息

Department of Immunology, Norman Bethune College of Medicine, Jilin University, Changchun 130021, P.R. China.

出版信息

Oncol Rep. 2013 Jul;30(1):260-8. doi: 10.3892/or.2013.2440. Epub 2013 Apr 30.

DOI:10.3892/or.2013.2440
PMID:23633115
Abstract

Mucin 1 (MUC1) is a large transmembrane glycoprotein that is aberrantly overexpressed in most adenocarcinomas and certain hematological malignancies. MUC1 is known to function as an oncogene with roles in both tumor formation and progression, making it a potential target for immunotherapy. B16-MUC1 cells with human full-length MUC1 are frequently used to study the antitumor activities of MUC1-based vaccines. However, we found that the growth of B16-MUC1 cells was significantly reduced in vitro. Therefore, in this study, we established two MUC1-positive clones, B16-MUC1 9-12 and B16-MUC1 9-23, and one empty vector control clone, B16-neo, to investigate the effects of MUC1 on the cancer-related characteristics of B16 cells in vitro and in vivo. Our results demonstrated that, compared with MUC1-negative cells, cells expressing MUC1 exhibited decreased cell proliferation, increased cell cycle arrest and reduced cell migratory and invasive capacities. We further investigated several MUC1-related molecules of the β-catenin pathway, and found that the expression of MUC1 decreased the translocation of β-catenin into the nucleus, reduced the activity of T cell factor (TCF) and blocked the expression of cyclin D1 and c-Myc. Moreover, when inoculated into BALB/c nude mice, cells expressing MUC1 developed smaller tumors compared with the control cells. These results demonstrate that MUC1 expression negatively affects the malignancy of B16 cells, and suggest that the regulatory mechanisms of MUC1 as an oncoprotein are more complex than previously appreciated.

摘要

黏蛋白 1(MUC1)是一种大型跨膜糖蛋白,在大多数腺癌和某些血液恶性肿瘤中异常过表达。MUC1 被认为是一种癌基因,在肿瘤形成和进展中都具有作用,使其成为免疫治疗的潜在靶点。具有全长人 MUC1 的 B16-MUC1 细胞常用于研究基于 MUC1 的疫苗的抗肿瘤活性。然而,我们发现 B16-MUC1 细胞的体外生长明显减少。因此,在这项研究中,我们建立了两个 MUC1 阳性克隆,B16-MUC1 9-12 和 B16-MUC1 9-23,以及一个空载体对照克隆 B16-neo,以研究 MUC1 对 B16 细胞体外和体内与癌症相关特征的影响。我们的结果表明,与 MUC1 阴性细胞相比,表达 MUC1 的细胞表现出细胞增殖减少、细胞周期停滞增加以及细胞迁移和侵袭能力降低。我们进一步研究了 β-连环蛋白途径的几个 MUC1 相关分子,发现 MUC1 的表达减少了 β-连环蛋白向核内的易位,降低了 T 细胞因子(TCF)的活性并阻断了细胞周期蛋白 D1 和 c-Myc 的表达。此外,当接种到 BALB/c 裸鼠中时,表达 MUC1 的细胞与对照细胞相比形成的肿瘤更小。这些结果表明 MUC1 表达负性影响 B16 细胞的恶性程度,并表明 MUC1 作为癌蛋白的调节机制比以前认为的更为复杂。

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Targeting MUC1 and JNK by RNA interference and inhibitor inhibit the development of hepatocellular carcinoma.通过RNA干扰和抑制剂靶向MUC1和JNK可抑制肝细胞癌的发展。
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Muc1 promotes migration and lung metastasis of melanoma cells.黏蛋白 1 促进黑色素瘤细胞的迁移和肺转移。
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Mucin 1 gene silencing inhibits the growth of SMMC-7721 human hepatoma cells through Bax-mediated mitochondrial and caspase-8-mediated death receptor apoptotic pathways.粘蛋白1基因沉默通过Bax介导的线粒体途径和半胱天冬酶-8介导的死亡受体凋亡途径抑制人肝癌SMMC-7721细胞的生长。
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