Genome-wide comparison of human keratinocyte and squamous cell carcinoma responses to UVB irradiation: implications for skin and epithelial cancer

Dazard, Jean-Eudes; Gal, Hilah; Amariglio, Ninette; Rechavi, Gideon; Domany, Eytan; Givol, David

doi:10.1038/sj.onc.1206537

Cited by 94 publications

(89 citation statements)

References 57 publications

(50 reference statements)

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“…As expected for a mutant p53 protein, no modification of its expression was found in response to cisplatin (Figure 6a). We found that while p73-mediated growth arrest and apoptotic target genes p21 waf1 , bax, p53AIP1, pig-3 were induced upon cisplatin treatment, S100A2 mRNA and protein, in agreement with previously reported findings (Dazard et al, 2003), were downregulated (Figure 6a-c). Similar findings were obtained upon treatment of HaCaT cells with doxorubicin (data not shown).…”

Section: S100a2 Expression Is Induced During Keratinocyte Differentiasupporting

confidence: 81%

S100A2 gene is a direct transcriptional target of p53 homologues during keratinocyte differentiation

Lapi¹,

Iovino²,

Fontemaggi³

et al. 2006

Oncogene

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The p53 paralogues p73, p63 and their respective truncated isoforms have been shown to be critical regulators of developmental and differentiation processes. Indeed, both p73-and p63-deficient mice exhibit severe developmental defects. Here, we show that S100A2 gene, whose transcript and protein are induced during keratinocyte differentiation of HaCaT cells, is a direct transcriptional target of p73b and DNp63a and is required for proper keratinocyte differentiation. Transactivation assays reveal that p73b and DNp63a exert opposite transcriptional effects on S100A2 gene. While DNp63a is found in vivo onto S100A2 regulatory regions predominantly in proliferating cells, p73b is recruited in differentiating cells. Silencing of p73 impairs the induction of S100A2 during the differentiation of HaCaT cells. Moreover, silencing of p73 or S100A2 impairs the proper expression of keratinocyte differentiation markers. Of note, p53 family members do not trigger S100A2 gene expression in response to apoptotic doses of cisplatin and doxorubicin.

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Section: S100a2 Expression Is Induced During Keratinocyte Differentiasupporting

confidence: 81%

S100A2 gene is a direct transcriptional target of p53 homologues during keratinocyte differentiation

Lapi¹,

Iovino²,

Fontemaggi³

et al. 2006

Oncogene

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“…Even in the absence of p53, the same gene size relationship exists for UV-induced genes (109). Compact p53-independent UV-induced genes included AP-1 responsive immediate early genes, NFjB-regulated cytokines and histones (1,29,48,55,168). Therefore, UV-induced genes tend to be compact, regardless of the transcription factor driving expression.…”

Section: Uv Ddr the Transcription Paradox And Gene Sizementioning

confidence: 95%

Post-Transcriptional Regulation of DNA Damage-Responsive Gene Expression

McKay

2014

Antioxidants & Redox Signaling

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Significance: Production of proteins requires the synthesis, maturation, and export of mRNAs before their translation in the cytoplasm. Endogenous and exogenous sources of DNA damage pose a challenge to the coordinated regulation of gene expression, because the integrity of the DNA template can be compromised by DNA lesions. Cells recognize and respond to this DNA damage through a variety of DNA damage responses (DDRs). Failure to deal with DNA damage appropriately can lead to genomic instability and cancer. Recent Advances: The p53 tumor suppressor plays a dominant role in DDR-dependent changes in gene expression, but this transcription factor is not solely responsible for all changes. Recent evidence indicates that RNA metabolism is integral to DDRs as well. In particular, post-transcriptional processes are emerging as important contributors to these complex responses. Critical Issues: Transcriptional, post-transcriptional, and translational regulation of gene expression is subject to changes in response to DNA damage. How these processes are intertwined in the unfolding of DDR is not fully understood. Future Directions: Many complex regulatory responses combine to determine cell fate after DNA damage. Understanding how transcriptional, post-transcriptional, and translational processes interdigitate to create a web of regulatory interactions will be one of the key challenges to fully understand DDRs. Antioxid. Redox Signal. 20, 640-654.

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“…Beside their constitutive expression in myeloid cells, they are expressed in epithelial cells in response to stress [14,15]. Their expression is transiently induced in keratinocytes after epidermal injury [16,17], after UVB irradiation [18], and in response to proinflammatory cytokines such as TNFa and IL1b [14]. Data showing that the two S100 proteins are up regulated by the putative TLR ligand LPS are conflicting [19,20].…”

Section: Introductionmentioning

confidence: 99%

Double‐stranded RNA induces S100 gene expression by a cycloheximide‐sensitive factor

et al. 2011

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Edited by Hans-Dieter Klenk Keywords:Cytokine burst Non-viral dsRNA Organotypic skin model Secondary response gene Tissue repair a b s t r a c t Viral double-stranded RNA (dsRNA) and its synthetic analog polyI:C are recognized via multiple pathways and induce the expression of genes related to inflammation. In the present study, we demonstrated the polyI:C-induced gene expression of the damage associated molecular pattern (DAMP) molecules S100A8 and S100A9, while other S100 genes were not affected. Cycloheximide and Brefeldin A treatment revealed both the expression of S100A8 and S100A9 as secondary response genes and the involvement of polyI:C-induced cytokines herein. Several type I and type III interferons such as IFNb, IL-20, IL-24, and IFNk/IL-29 were expressed in response to polyI:C, however, they failed to induce S100A8 and S100A9 gene expression. These data indicate the involvement of the danger molecule S100A8/A9 in the resistance against viruses.

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Genome-wide comparison of human keratinocyte and squamous cell carcinoma responses to UVB irradiation: implications for skin and epithelial cancer

Cited by 94 publications

References 57 publications

S100A2 gene is a direct transcriptional target of p53 homologues during keratinocyte differentiation

S100A2 gene is a direct transcriptional target of p53 homologues during keratinocyte differentiation

Post-Transcriptional Regulation of DNA Damage-Responsive Gene Expression

Double‐stranded RNA induces S100 gene expression by a cycloheximide‐sensitive factor

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