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GATA转录因子与癌症

GATA Transcription Factors and Cancer.

作者信息

Zheng Rena, Blobel Gerd A

机构信息

Division of Hematology, The Children's Hospital of Philadelphia, Philadelphia, PA, USA.

出版信息

Genes Cancer. 2010 Dec;1(12):1178-88. doi: 10.1177/1947601911404223.

Abstract

It has been almost a quarter century since it was first appreciated that a class of oncogenes contained in rapidly transforming avian retroviruses encoded DNA-binding transcription factors. As with other oncogenes, genetic recombination with the viral genome led to their overexpression or functional alteration. In the years that followed, alterations of numerous transcription factors were shown to be causatively involved in various cancers in human patients and model organisms. Depending on their normal cellular functions, these factors were subsequently categorized as proto-oncogenes or tumor suppressor genes. This review focuses on the role of GATA transcription factors in carcinogenesis. GATA factors are zinc finger DNA binding proteins that control the development of diverse tissues by activating or repressing transcription. GATA factors thus coordinate cellular maturation with proliferation arrest and cell survival. Therefore, a role of this family of genes in human cancers is not surprising. Prominent examples include structural mutations in GATA1 that are found in almost all megakaryoblastic leukemias in patients with Down syndrome; loss of GATA3 expression in aggressive, dedifferentiated breast cancers; and silencing of GATA4 and GATA5 expression in colorectal and lung cancers. Here, we discuss possible mechanisms of carcinogenesis vis-à-vis the normal functions of GATA factors as they pertain to human patients and mouse models of cancer.

摘要

人们首次认识到快速转化的禽逆转录病毒中所含的一类癌基因编码DNA结合转录因子,至今已近四分之一个世纪。与其他癌基因一样,与病毒基因组的基因重组导致它们过度表达或功能改变。在随后的几年里,大量转录因子的改变被证明与人类患者和模式生物的各种癌症有因果关系。根据它们正常的细胞功能,这些因子随后被归类为原癌基因或肿瘤抑制基因。本综述聚焦于GATA转录因子在致癌作用中的作用。GATA因子是锌指DNA结合蛋白,通过激活或抑制转录来控制多种组织的发育。因此,GATA因子协调细胞成熟与增殖停滞和细胞存活。因此,这个基因家族在人类癌症中发挥作用并不奇怪。突出的例子包括唐氏综合征患者几乎所有巨核细胞白血病中发现的GATA1结构突变;侵袭性、去分化乳腺癌中GATA3表达缺失;以及结直肠癌和肺癌中GATA4和GATA5表达沉默。在这里,我们讨论了与GATA因子在人类患者和癌症小鼠模型中的正常功能相关的致癌作用的可能机制。

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