2007
DOI: 10.1093/carcin/bgm258
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Properties of the six isoforms of p63: p53-like regulation in response to genotoxic stress and cross talk with ΔNp73

Abstract: TP63, a member of the TP53 gene family, encodes two groups of three isoforms (alpha, beta and gamma). The TAp63 isoforms act as transcription factors. The DeltaNp63 isoforms lack the main transcription activation domain and act as dominant-negative inhibitors of transactivation (TA) isoforms. To clarify the role of these isoforms and to better understand their functional overlap with p53, we ectopically expressed each p63 isoform in the p53-null hepatocellular carcinoma cell line Hep3B. All TA isoforms, as wel… Show more

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Cited by 81 publications
(94 citation statements)
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“…Plasmids and mutagenesis DNp63a, DN89 b-catenin mutant and DNTCF4-expression vectors have been previously described Cavard et al, 2006;Petitjean et al, 2008). pCMV-p53-expression vector was from Clontech (Mountain View, CA, USA).…”
Section: Methodsmentioning
confidence: 99%
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“…Plasmids and mutagenesis DNp63a, DN89 b-catenin mutant and DNTCF4-expression vectors have been previously described Cavard et al, 2006;Petitjean et al, 2008). pCMV-p53-expression vector was from Clontech (Mountain View, CA, USA).…”
Section: Methodsmentioning
confidence: 99%
“…Luciferase assays were performed as previously described (Petitjean et al, 2008), by using 1.8 mg of p53, DNp63a, wildtype or mutant b-catenin-expression vectors, 1 mg of luciferase reporter plasmid, and 0.1 mg of renilla luciferase control plasmid. b-catenin-DNp63 axis in tumour progression C Ruptier et al…”
Section: Luciferase Assaysmentioning
confidence: 99%
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“…TAp63g is the most active form at transcriptional level and accumulates in a phosphorylated form during DNA damage (by doxorubicin) with a drastically prolonged half-life. 113 This implies a role for TAp63 in DNA damage responses, as for example shown in the ovary, see also the section 'Protecting fertility following chemotherapy'.…”
Section: Np63mentioning
confidence: 99%
“…6 Recently, in vitro studies have also shown that ⌬Np63 isoforms inhibit TAp63 isoforms in a dose-dependent manner. 7 In addition to their role in normal development, a potential role for p63 proteins in tumorigenesis is supported by the finding that p63 immunoreactivity is observed in more than 90% of squamous epithelial malignancies. 8 However, because of the lack of reliable antibodies for ⌬N and TAp63, the p63 isoforms expressed in these malignant lesions were not determined in most studies.…”
mentioning
confidence: 96%