New p63 targets in keratinocytes identified by a genome-wide approach

Viganò, M. Alessandra; Lamartine, Jérôme; Testoni, Barbara; Merico, Daniele; Alotto, Daniela; Castagnoli, Carlotta; Robert, Amélie; Candi, Eleonora; Melino, Gerry; Gidrol, Xavier; Mantovani, Roberto

doi:10.1038/sj.emboj.7601375

Cited by 107 publications

(142 citation statements)

References 59 publications

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“…The accepted activity was its dominant negative effect exerted towards the TAp63 isoform, as suggested by co-transfection experiments in luciferase reporter assays [3]. However, in addition to the competition between TAp63 and Np63 isoforms, growing evidence indicated that these N-terminal isoforms had different transcriptional specificities a specificity confirmed by functional domain characterization [32][33][34], and microarray analysis showing that both isoforms can induce gene transcription [35,29]. As expected from genes important for developmental and differentiation processes, the more strongly represented classes of target genes are those concerned with cell adhesion, the cytoskeleton, and the cell cycle.…”

Section: Transcriptional Activities Of P63 Isoformsmentioning

confidence: 97%

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p63 in epithelial development

Candi

Cipollone

Cervo

et al. 2008

Cell. Mol. Life Sci.

121

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List of abbreviations: K, keratin; p63-/-, mouse knockout for p63; p63-/-;TA, p63 knockout mice complemented with TAp63; p63-/-;ΔN, p63 knockout mice complemented with ΔNp63; p63-/-;TA;ΔN, p63 knockout mice complemented with both TAp63 and ΔNp63;IKKα, IkB kinase-α; TA, transactivation domain; ΔN, amino-terminal truncated protein. AbstractThe epidermis, the outer layer of the skin composed of keratinocytes, is a stratified epithelium that functions as a barrier to protect the organism from dehydration and external insults. The epidermis develops following the action of the transcription factor p63, a member of the p53 family of transcription factors. The Trp63 gene contains two promoters, driving the production of distinct proteins, one with an N-terminal transactivation domain (TAp63) and one without (DeltaNp63), although their relative contribution to epidermal development is not clearly established. Trp63 mutations are involved in the pathogenesis of several human diseases, phenotypically characterized by ectodermal dysplasia. In this review we summarise the current advances that have been made in understanding the role of p63 in epidermal morphogenesis.

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Section: Transcriptional Activities Of P63 Isoformsmentioning

confidence: 97%

“…In this context, a genomewide approach led to the identification of several high-confidence target genes for Np63 [35] However, only a few of these have been demonstrated to have a defined impact on epidermal formation and differentiation in vivo.…”

Section: Transcriptional Activities Of P63 Isoformsmentioning

confidence: 99%

p63 in epithelial development

Candi

Cipollone

Cervo

et al. 2008

Cell. Mol. Life Sci.

121

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“…HaCaT cells and first passage primary human adult keratinocytes (haKCs), derived from healthy individuals (breast skin biopsies), were grown and handled as previously described (Vigano`et al, 2006). Maintenance, differentiation and transfection of primary human neonatal keratinocytes (hnKCs; CellNtec, CH) were conducted as previously described (Pozzi et al, 2009).…”

Section: Cell Culture and Transfectionsmentioning

confidence: 99%

“…Immunofluorescence analysis of frozen human adult-thigh skin sections and cultured cells was performed as previously described (Vigano`et al, 2006) with anti-p63, anti-KLF4 (Genespin, I) and anti-KRT1 (Covance, Princeton, NJ, USA) antibodies. Nuclei were counterstained with 4 0 ,6-diamidino-2-phenylindole (DAPI).…”

Section: Immunofluorescence Analysismentioning

confidence: 99%

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Mutant p53 subverts p63 control over KLF4 expression in keratinocytes

et al. 2010

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Genetic experiments established that p63 is crucial for the development and maintenance of pluri-stratified epithelia and KLF4 for the barrier function of the skin. KLF4 is one of the factors that reprogram differentiated cells to iPS. We investigated the relationship between p63 and KLF4 using RNA interference, overexpression, chromatin immunoprecipitation and transient transfections with reporter constructs. We find that p63 directly represses KLF4 in normal keratinocytes (KCs) by binding to upstream promoter sites. Unlike p63, KLF4 levels are high in the upper layers of human skin and increase upon differentiation of KCs in vitro. In HaCaT KCs, which harbor two mutant alleles of p53, inactivation of p63 and of mutant p53 leads to KLF4 repression. p63 and p53 mutants are bound to sites in the KLF4 core promoter. Importantly, expression of the H179Y and R282Q p53 mutants in primary KCs is sufficient to activate endogenous KLF4. Finally, immunohistochemical analysis of tissue arrays confirms increased coexpression of KLF4 and mutant p53 in squamous cell carcinomas. Our data indicate that suppression of KLF4 is part of the growth-promoting strategy of p63 in the lower layers of normal epidermis, and that tumor-predisposing p53 mutations hijack p63 to a different location on the promoter, turning it into an activator of this reprogramming factor.

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