卵巢癌中TCF/β-连环蛋白通路的罕见激活

Rare activation of the TCF/beta-catenin pathway in ovarian cancer.

作者信息

Furlong M T, Morin P J

机构信息

Laboratory of Biological Chemistry, Gerontology Research Center, National Institute on Aging, Baltimore, Maryland 21224, USA.

出版信息

Gynecol Oncol. 2000 Apr;77(1):97-104. doi: 10.1006/gyno.1999.5718.

DOI:10.1006/gyno.1999.5718

PMID:10739697

Abstract

OBJECTIVE

The activation of the T cell factor/beta-catenin pathway is a crucial event in colon cancer initiation. A recent report describing the presence of beta-catenin mutations in endometrioid ovarian cancer suggested that the TCF/beta-catenin pathway may be generally activated in ovarian cancer. We therefore undertook to determine the frequency of activation of this pathway in ovarian cancer cell lines using a functional screen.

METHODS

We functionally screened a series of ovarian cancer cell lines for the presence of constitutive TCF/beta-catenin-mediated transcriptional activity using a reporter assay. Lines possessing such activity were subjected to mutational and gel-shift analysis, as well as sensitivity to the introduction of dominant-negative TCF or APC alleles. A cDNA harboring a beta-catenin point mutation found in an ovarian cancer line was incorporated into an expression plasmid for functional analysis.

RESULTS

Constitutive TCF/beta-catenin transcriptional activity was detected in 21% (4 of 19) of ovarian lines studied, while 32% (6 of 19) exhibited greater than twofold repression. One of the constitutively active lines, UCI107, harbored an activating beta-catenin point mutation, which was shown to be capable of inducing TCF/beta-catenin transcriptional activity in transiently transfected 293 cells. A second active line, SW626, was shown to harbor an inactivating APC mutation and may in fact be of colonic origin. The third and fourth lines harbored neither an APC nor a beta-catenin mutation. Gel-shift analysis, together with the absence of sensitivity to dominant-negative TCF, indicated that the reporter activity exhibited by the latter two cell lines may not be due to a TCF/beta-catenin transcriptional complex.

CONCLUSIONS

These results indicate that genuine constitutive activation of the TCF/beta-catenin pathway is infrequent in ovarian cancer, but that constitutive transcriptional repression from TCF sites is more common in this tumor type.

摘要

目的

T细胞因子/β-连环蛋白信号通路的激活是结肠癌起始过程中的关键事件。最近一份关于子宫内膜样卵巢癌中存在β-连环蛋白突变的报告表明，TCF/β-连环蛋白信号通路可能在卵巢癌中普遍被激活。因此，我们通过功能筛选来确定该信号通路在卵巢癌细胞系中的激活频率。

方法

我们使用报告基因检测法对一系列卵巢癌细胞系进行功能筛选，以检测是否存在组成型TCF/β-连环蛋白介导的转录活性。具有这种活性的细胞系进行了突变和凝胶迁移分析，以及对导入显性负性TCF或APC等位基因的敏感性分析。将在一个卵巢癌细胞系中发现的携带β-连环蛋白点突变的cDNA插入表达质粒进行功能分析。

结果

在所研究的19个卵巢癌细胞系中，21%（4/19）检测到组成型TCF/β-连环蛋白转录活性，而32%（6/19）表现出两倍以上的抑制。其中一个组成型激活的细胞系UCI107携带一个激活型β-连环蛋白点突变，该突变在瞬时转染的293细胞中能够诱导TCF/β-连环蛋白转录活性。另一个激活的细胞系SW626携带一个失活的APC突变，实际上可能起源于结肠。第三和第四个细胞系既没有APC突变也没有β-连环蛋白突变。凝胶迁移分析以及对显性负性TCF不敏感表明，后两个细胞系表现出的报告基因活性可能不是由于TCF/β-连环蛋白转录复合物。