The ΔNp63α Phosphoprotein Binds the p21 and 14-3-3σ Promoters In Vivo and Has Transcriptional Repressor Activity That Is Reduced by Hay-Wells Syndrome-Derived Mutations

Westfall, Matthew D.; Mays, Deborah J.; Sniezek, Joseph C.; Pietenpol, Jennifer A.

doi:10.1128/mcb.23.7.2264-2276.2003

Cited by 319 publications

(414 citation statements)

References 52 publications

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“…In addition, repression of 14-3-3s expression was seen by a tumor-associated p63 splice variant (Delta Np63) in vitro. 34,35 However, again no correlation was found between the p63 status and 14-3-3s expression in hyperproliferative skin disease. 20 These studies all suggest independence of 14-3-3s expression of p53 and its homologues p63 and p73.…”

Section: Discussionmentioning

confidence: 94%

Downregulation of 14-3-3σ in ovary, prostate and endometrial carcinomas is associated with CpG island methylation

et al. 2005

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Section: Discussionmentioning

confidence: 94%

Downregulation of 14-3-3σ in ovary, prostate and endometrial carcinomas is associated with CpG island methylation

et al. 2005

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“…In the p63 ChIP, we observed significant enrichment for the putative PTPN14 and ING1 REs relative to background (Figure 4b). Constitutive p63 binding was also observed at the known p63-responsive elements p21 site 1 (Westfall et al, 2003) and JAG1 (Sasaki et al, 2002). After ADR treatment, p63 binding to all four REs decreased.…”

Section: Endogenous P63 Binds Intronic Res In the Ptpn14 And Ing1 Genesmentioning

confidence: 85%

“…As a source for p53, H1299 cells were transiently transfected with pCEP4 or pCEP4-p53 expression vectors. Immunoprecipitations were carried out as described previously (Westfall et al, 2003), using an a-myc antibody for myc-DNp63a and a combination of the PAb1801 (Santa Cruz, Santa Cruz, CA, USA) and PAb421 (Calbiochem, San Diego, CA, USA) antibodies for p53.…”

Section: Immunopurificationmentioning

confidence: 99%

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p63 consensus DNA-binding site: identification, analysis and application into a p63MH algorithm

et al. 2007

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p53 and p63 belong to a family of sequence-specific transcription factors regulating key cellular processes. Differential composition of the p53 and p63 DNA-binding sites may contribute to distinct functions of these protein homologues. We used SELEX (systematic evolution of ligands by exponential enrichment) methodology to identify nucleic acid ligands for p63. We found that p63 bound preferentially to DNA fragments conforming to the 20 bp sequence 5 0 -RRRC(A/G)(A/T)GYYYRRRC(A/T) (C/T)GYYY-3 0 . Relative to the p53 consensus, the p63 consensus DNA-binding site (DBS) was more degenerate, particularly at positions 10 and 11, and was enriched for A/G at position 5 and C/T at position 16 of the consensus. The differences in DNA-binding site preferences between p63 and p53 influenced their ability to activate transcription from select response elements (REs) in cells. A computer algorithm, p63MH, was developed to find candidate p63-binding motifs on input sequences. We identified genes responsive to p63 regulation that contain functional p63 REs. Our results suggest that the sequence composition of REs could be one contributing factor to target gene discrimination between p63 and p53.

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“…14-3-3 is expressed exclusively in epithelial cells and induces cell cycle arrest (Hermeking et al, 1997). ⌬Np63␣ binds directly to the p21 WAF/Cip1 and 14-3-3 promoters (Westfall et al, 2003) and inhibits their transcription, thus favoring cell proliferation. Another mechanism by which ⌬Np63 isoforms may promote proliferative potential is to counteract the antiproliferative activity of TAp63␥ (see Fig.…”

Section: P63-in the Beginningmentioning

confidence: 99%

Proliferation and cornification during development of the mammalian epidermis

2005

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The ΔNp63α Phosphoprotein Binds the p21 and 14-3-3σ Promoters In Vivo and Has Transcriptional Repressor Activity That Is Reduced by Hay-Wells Syndrome-Derived Mutations

Cited by 319 publications

References 52 publications

Downregulation of 14-3-3σ in ovary, prostate and endometrial carcinomas is associated with CpG island methylation

Downregulation of 14-3-3σ in ovary, prostate and endometrial carcinomas is associated with CpG island methylation

p63 consensus DNA-binding site: identification, analysis and application into a p63MH algorithm

Proliferation and cornification during development of the mammalian epidermis

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