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鉴定 TFAP2C 在激素反应性乳腺癌细胞中的主要靶基因。

Identification of primary gene targets of TFAP2C in hormone responsive breast carcinoma cells.

机构信息

Department of Surgery, University of Iowa Carver College of Medicine, Iowa City, IA 52242, USA.

出版信息

Genes Chromosomes Cancer. 2010 Oct;49(10):948-62. doi: 10.1002/gcc.20807.

Abstract

The TFAP2C transcription factor is involved in mammary development, differentiation, and oncogenesis. Previous studies established a role for TFAP2C in the regulation of ESR1 (ERalpha) and ERBB2 (Her2) in breast carcinomas. However, the role of TFAP2C in different breast cancer phenotypes has not been examined in detail. To develop a more complete characterization of TFAP2C target genes, ChIP-seq with anti-TFAP2C antibody and expression arrays with TFAP2C knock down were analyzed in MCF-7 breast carcinoma cells. Genomic sequences common to the ChIP-seq data set defined the consensus sequence for TFAP2C chromatin binding as the nine base sequence SCCTSRGGS (S = G/C, r = A/G), which closely matches the previously defined optimal in vitro binding site. Comparing expression arrays before and after knock down of TFAP2C with ChIP-seq data demonstrated a conservative estimate that 8% of genes altered by TFAP2C expression are primary target genes and includes genes that are both induced and repressed by TFAP2C. A set of 447 primary target genes of TFAP2C was identified, which included ESR1 (ERalpha), FREM2, RET, FOXA1, WWOX, GREB1, MYC, and members of the retinoic acid response pathway. The identification of ESR1, WWOX, GREB1, and FOXA1 as primary targets confirmed the role of TFAP2C in hormone response. TFAP2C plays a critical role in gene regulation in hormone responsive breast cancer and its target genes are different than for the Her2 breast cancer phenotype.

摘要

TFAP2C 转录因子参与乳腺发育、分化和肿瘤发生。先前的研究确立了 TFAP2C 在调节乳腺癌中的 ESR1(ERalpha)和 ERBB2(Her2)中的作用。然而,TFAP2C 在不同乳腺癌表型中的作用尚未详细研究。为了更全面地描述 TFAP2C 靶基因,我们在 MCF-7 乳腺癌细胞中分析了抗 TFAP2C 抗体的 ChIP-seq 和 TFAP2C 敲低的表达谱。ChIP-seq 数据集共有的基因组序列定义了 TFAP2C 染色质结合的共有序列为 SCCTSRGGS(S = G/C,r = A/G),这与先前定义的最佳体外结合位点非常吻合。在 TFAP2C 表达敲低前后与 ChIP-seq 数据比较表达谱表明,保守估计 8%的基因改变由 TFAP2C 表达引起,这些基因包括 TFAP2C 诱导和抑制的基因。确定了一组 447 个 TFAP2C 的初级靶基因,其中包括 ESR1(ERalpha)、FREM2、RET、FOXA1、WWOX、GREB1、MYC 和视黄酸反应途径的成员。ESR1、WWOX、GREB1 和 FOXA1 作为初级靶基因的鉴定证实了 TFAP2C 在激素反应中的作用。TFAP2C 在激素反应性乳腺癌的基因调控中起着关键作用,其靶基因与 Her2 乳腺癌表型不同。

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