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Sp1 transcription factor: A long-standing target in cancer chemotherapy

转录因子Sp1 发起人 生物 基因 转录因子 DNA结合蛋白 癌变 遗传学 抄写(语言学) 基因表达 细胞生物学 癌症研究 语言学 哲学
作者
Carolina Vizcaíno,Sylvia Mansilla,José Portugal
出处
期刊:Pharmacology & Therapeutics [Elsevier BV]
卷期号:152: 111-124 被引量:462
标识
DOI:10.1016/j.pharmthera.2015.05.008
摘要

Sp1 (specificity protein 1) is a well-known member of a family of transcription factors that also includes Sp2, Sp3 and Sp4, which are implicated in an ample variety of essential biological processes and have been proven important in cell growth, differentiation, apoptosis and carcinogenesis. Sp1 activates the transcription of many cellular genes that contain putative CG-rich Sp-binding sites in their promoters. Sp1 and Sp3 proteins bind to similar, if not the same, DNA tracts and compete for binding, thus they can enhance or repress gene expression. Evidences exist that the Sp-family of proteins regulates the expression of genes that play pivotal roles in cell proliferation and metastasis of various tumors. In patients with a variety of cancers, high levels of Sp1 protein are considered a negative prognostic factor. A plethora of compounds can interfere with the trans-activating activities of Sp1 and other Sp proteins on gene expression. Several pathways are involved in the down-regulation of Sp proteins by compounds with different mechanisms of action, which include not only the direct interference with the binding of Sp proteins to their putative DNA binding sites, but also promoting the degradation of Sp protein factors. Down-regulation of Sp transcription factors and Sp1-regulated genes is drug-dependent and it is determined by the cell context. The acknowledgment that several of those compounds are safe enough might accelerate their introduction into clinical usage in patients with tumors that over-express Sp1.
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