Regulation of MYC gene expression by aberrant Wnt/β-catenin signaling in colorectal cancer.

Sherri A. Rennoll, G. Yochum
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引用次数: 120

Abstract

The Wnt/β-catenin signaling pathway controls intestinal homeostasis and mutations in components of this pathway are prevalent in human colorectal cancers (CRCs). These mutations lead to inappropriate expression of genes controlled by Wnt responsive DNA elements (WREs). T-cell factor/Lymphoid enhancer factor transcription factors bind WREs and recruit the β-catenin transcriptional co-activator to activate target gene expression. Deregulated expression of the c-MYC proto-oncogene (MYC) by aberrant Wnt/β-catenin signaling drives colorectal carcinogenesis. In this review, we discuss the current literature pertaining to the identification and characterization of WREs that control oncogenic MYC expression in CRCs. A common theme has emerged whereby these WREs often map distally to the MYC genomic locus and control MYC gene expression through long-range chromatin loops with the MYC proximal promoter. We propose that by determining which of these WREs is critical for CRC pathogenesis, novel strategies can be developed to treat individuals suffering from this disease.
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结直肠癌中Wnt/β-catenin异常信号对MYC基因表达的调控
Wnt/β-catenin信号通路控制肠道稳态,该通路组分的突变在人类结直肠癌(crc)中普遍存在。这些突变导致Wnt反应性DNA元件(WREs)控制的基因不适当表达。t细胞因子/淋巴细胞增强因子转录因子结合WREs并募集β-catenin转录共激活因子激活靶基因表达。异常Wnt/β-catenin信号通路介导的c-MYC原癌基因(MYC)表达失调驱动结直肠癌的发生。在这篇综述中,我们讨论了目前有关在crc中控制致癌MYC表达的WREs的鉴定和表征的文献。一个共同的主题已经出现,即这些WREs通常远端映射到MYC基因组位点,并通过MYC近端启动子的远程染色质环控制MYC基因表达。我们建议,通过确定这些WREs中哪些对结直肠癌的发病机制至关重要,可以开发新的策略来治疗患有这种疾病的个体。
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