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Overexpression of Transcription Factor Sp1 Leads to Gene Expression Perturbations and Cell Cycle Inhibition

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TLDR
It is shown that the binding to DNA of overexpressed Sp1 induces an inhibition of cell cycle progression that precedes apoptosis and a transcriptional response targeting genes containing Sp1 binding sites in their promoter or not suggesting both direct Sp1-driven transcription and indirect mechanisms.
Abstract
BACKGROUND: The ubiquitous transcription factor Sp1 regulates the expression of a vast number of genes involved in many cellular functions ranging from differentiation to proliferation and apoptosis. Sp1 expression levels show a dramatic increase during transformation and this could play a critical role for tumour development or maintenance. Although Sp1 deregulation might be beneficial for tumour cells, its overexpression induces apoptosis of untransformed cells. Here we further characterised the functional and transcriptional responses of untransformed cells following Sp1 overexpression. METHODOLOGY AND PRINCIPAL FINDINGS: We made use of wild-type and DNA-binding-deficient Sp1 to demonstrate that the induction of apoptosis by Sp1 is dependent on its capacity to bind DNA. Genome-wide expression profiling identified genes involved in cancer, cell death and cell cycle as being enriched among differentially expressed genes following Sp1 overexpression. In silico search to determine the presence of Sp1 binding sites in the promoter region of modulated genes was conducted. Genes that contained Sp1 binding sites in their promoters were enriched among down-regulated genes. The endogenous sp1 gene is one of the most down-regulated suggesting a negative feedback loop induced by overexpressed Sp1. In contrast, genes containing Sp1 binding sites in their promoters were not enriched among up-regulated genes. These results suggest that the transcriptional response involves both direct Sp1-driven transcription and indirect mechanisms. Finally, we show that Sp1 overexpression led to a modified expression of G1/S transition regulatory genes such as the down-regulation of cyclin D2 and the up-regulation of cyclin G2 and cdkn2c/p18 expression. The biological significance of these modifications was confirmed by showing that the cells accumulated in the G1 phase of the cell cycle before the onset of apoptosis. CONCLUSION: This study shows that the binding to DNA of overexpressed Sp1 induces an inhibition of cell cycle progression that precedes apoptosis and a transcriptional response targeting genes containing Sp1 binding sites in their promoter or not suggesting both direct Sp1-driven transcription and indirect mechanisms.

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Posted ContentDOI

Distinct genomic and epigenomic features demarcate hypomethylated blocks in colon cancer

TL;DR: The analyses suggest that the overall architecture of HMBs is guided by pre-existing chromatin architecture, and are associated with aberrant activity of promoter-like sequences at the boundary, significantly coincide with the boundaries of Topologically Associating Domains of the chromatin.
Journal ArticleDOI

Distinct genomic and epigenomic features demarcate hypomethylated blocks in colon cancer.

TL;DR: The analyses suggest that the overall architecture of HMBs is guided by pre-existing chromatin architecture, and are associated with aberrant activity of promoter-like sequences at the boundary, and significantly coincide with the boundaries of Topologically Associating Domains of the chromatin.
References
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Journal ArticleDOI

The Bcl-2 family: roles in cell survival and oncogenesis.

TL;DR: Current views of how the Bcl-2 family of anti- and proapoptotic regulators sense stress, interact with their relatives, perturb organelles such as the mitochondrion and endoplasmic reticulum and govern pathways to caspase activation are summarized.
Journal ArticleDOI

Sp1 and Krüppel-like factor family of transcription factors in cell growth regulation and cancer

TL;DR: The Sp/KLF family contains at least twenty identified members which include Sp1‐4 and numerous krüppel‐like factors; thus, the family is involved in several aspects of tumorigenesis.
Journal ArticleDOI

The many faces of metalloproteases: cell growth, invasion, angiogenesis and metastasis

TL;DR: Recent progress in identifying an essential role for metalloproteases in axon outgrowth is discussed, as an example of a focal invasive event, and the evolving concept of how MMPs might regulate stem cell fate during tumor development is discussed.
Journal ArticleDOI

A tale of three fingers: the family of mammalian Sp/XKLF transcription factors

TL;DR: Recent advances that have been directed towards understanding the biological role of transcription factors are summarized and discussed.
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