TA-p63-γ regulates expression of ΔN-p63 in a manner that is sensitive to p53

Li, N; Li, H; Cherukuri, Pratima; Farzan, Shohreh F.; Harmes, David C.; DiRenzo, James

doi:10.1038/sj.onc.1209270

Cited by 29 publications

(22 citation statements)

References 36 publications

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“…Both positive and negative regulation of DNp63 mRNA and protein have been shown by different groups to be mediated by both p53 and DNp63 itself (Harmes et al, 2003;Waltermann et al, 2003;Antonini et al, 2006;Romano et al, 2006). DNp63 may also be positively regulated by TAp63g in a manner that is independent of p53, suggesting yet another possible feedback mechanism (Li et al, 2006). Additional feedback mechanisms with potential relevance to human cancer have been proposed and involve distinct p63 target genes.…”

Section: Upstream Regulation Of P63 and P73 Transcriptionmentioning

confidence: 99%

p63 and p73 in human cancer: defining the network

2007

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The p53-related genes p63 and p73 exhibit significant structural homology to p53; however, they do not function as classical tumor suppressors and are rarely mutated in human cancers. Both p63 and p73 exhibit tissue-specific roles in normal development and a complex contribution to tumorigenesis that is due to their expression as multiple protein isoforms. The predominant p63/p73 isoforms expressed both in normal development and in many tumors lack the conserved transactivation (TA) domain; these isoforms instead exhibit a truncated N-terminus (DN) and function at least in part as transcriptional repressors. p63 and p73 isoforms are regulated through both transcriptional and post-translational mechanisms, and they in turn regulate diverse cellular functions including proliferation, survival and differentiation. The net effect of p63/p73 expression in a given context depends on the ratio of TA/DN isoforms expressed, on physical interaction between p63 and p73 isoforms, and on functional interactions with p53 at the promoters of specific downstream target genes. These multifaceted interactions occur in diverse ways in tumor-specific contexts, demonstrating a functional 'p53 family network' in human tumorigenesis. Understanding the regulation and mechanistic contributions of p63 and p73 in human cancers may ultimately provide new therapeutic opportunities for a variety of these diseases.

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Section: Upstream Regulation Of P63 and P73 Transcriptionmentioning

confidence: 99%

p63 and p73 in human cancer: defining the network

2007

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“…Moreover, ΔNp63 is recruited to and can activate its own promoter, thus providing an autoregulatory loop of self-regulation [28,83]. Importantly, loss of p53 leads to the stabilization of TAp63γ [84]. Consequently, disruption of TAp63γ expression leads to decreased expression of ΔNp63, and overexpression of TAp63γ enhances the activity of the ΔNp63 promoter.…”

Section: Tumor Suppressor or Oncogenic Role? Crosstalk Between P53 Famentioning

confidence: 99%

The role of P63 in cancer, stem cells and cancer stem cells

Nekulova

Holcakova

Coates

et al. 2011

Cellular and Molecular Biology Letters

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The transcription factor p63 has important functions in tumorigenesis, epidermal differentiation and stem cell self-renewal. The TP63 gene encodes multiple protein isoforms that have different or even antagonistic roles in these processes. The balance of p63 isoforms, together with the presence or absence of the other p53 family members, p73 and p53, has a striking biological impact. There is increasing evidence that interactions between p53-family members, whether cooperative or antagonistic, are involved in various cell processes. This review summarizes the current understanding of the role of p63 in tumorigenesis, metastasis, cell migration and senescence. In particular, recent data indicate important roles in adult stem cell and cancer stem cell regulation and in the response of cancer cells to therapy.

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“…32,10 Though little is known about the biological functions of TRAF4, our results indicate that the localization of the TRAF4 protein is associated with histological differentiation of SCCHN and that p63 cooperating with TRAF4 might be involved in the kerati- nocyte differentiation pathway. Since TRAF4 is also transactivated by p53 and TAp73, and as p53 family members are known to interact physically and functionally, 33,34 the in vivo regulation of TRAF4 expression is highly complex and tissue specific. In addition, TRAF4 localizes to the nuclei in all normal oral epithelial cells but this localization is disturbed in poorly differentiated SCCHN cells, indicating the existence of tumor-specific factors that regulate the intracellular distribution of TRAF4 in this tumor type.…”

Section: Discussionmentioning

confidence: 99%

TRAF4 is potently induced by TAp63 isoforms and localised according to differentiation in SCCHN

Coates²,

MacCallum³

et al. 2007

Cancer Biology & Therapy

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AbstrActp63, a member of the p53 family, is overexpressed in squamous cell carcinoma of the head and neck (SCCHN) and some other tumors of epithelial origin. As a transcription factor, p63 can bind to p53-type response elements and there is some overlap between p53 family transcriptional targets. Tumor necrosis factor receptor associated factor 4 (TRAF4) is a p53 regulated gene which is overexpressed in many human carcinomas. We investigated the involvement of p63 in regulation of TRAF4 and the expression of the TRAF4 protein in SCCHN. Disrupting endogenous p63 expression resulted in downregulation of TRAF4 mRNA and protein in an SCCHN cell line. Endogenous p63 bound to the TRAF4 promoter in vivo and reporter assays showed that p63, p73 and p53 can all transactivate TRAF4, with TAp63 isoforms being the most potent activators. The level of TRAF4 activation by TAp63 was two-fold higher than by p53, and TRAF4 was ten-fold more responsive to TAp63 than another p63-target, IGFBP3. Nuclear expression of TRAF4 was seen in normal oral epithelium and highly/moderately differentiated SCCHN, whereas cytoplasmic expression of TRAF4 was seen in poorly differentiated SCCHN. These results indicate that TRAF4 is a common target of p53 family members and that localization of TRAF4 is associated with differentiation of SCCHN cells.

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TA-p63-γ regulates expression of ΔN-p63 in a manner that is sensitive to p53

Cited by 29 publications

References 36 publications

p63 and p73 in human cancer: defining the network

p63 and p73 in human cancer: defining the network

The role of P63 in cancer, stem cells and cancer stem cells

TRAF4 is potently induced by TAp63 isoforms and localised according to differentiation in SCCHN

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