ΔNp63 Versatilely Regulates a Broad<i>NF-κB</i>Gene Program and Promotes Squamous Epithelial Proliferation, Migration, and Inflammation

Yang, Xinping; Lü, Hai; Yan, Bin; Romano, Rose Anne; Bian, Yansong; Friedman, Jay; Duggal, Praveen; Allen, Clint; Chuang, Ryan; Ehsanian, Reza; Si, Han; Sinha, Satrajit; Waes, Carter Van; Chen, Zhong

doi:10.1158/0008-5472.can-10-3445

Cited by 121 publications

(152 citation statements)

References 46 publications

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“…Indeed, loss of function of ΔNp63 enhances terminal maturation in stratified squamous epithelium (41). On one hand, ΔNp63α overexpression has been shown in a rat cell line to accelerate tumor growth in nude mice (42), and transgenic mice overexpressing ΔNp63α develop epidermal hyperplasia (43). Tp63 was recently shown to be required for maintenance of tumors, as inducible genetic deletion of all its isoforms led to blockade of chemically induced SCC formation in mice (44).…”

Section: Figurementioning

confidence: 99%

SOX2 and p63 colocalize at genetic loci in squamous cell carcinomas

Watanabe¹,

Ma²,

Peng³

et al. 2014

J. Clin. Invest.

141

150

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The transcription factor SOX2 is an essential regulator of pluripotent stem cells and promotes development and maintenance of squamous epithelia. We previously reported that SOX2 is an oncogene and subject to highly recurrent genomic amplification in squamous cell carcinomas (SCCs). Here, we have further characterized the function of SOX2 in SCC. Using ChIP-seq analysis, we compared SOX2-regulated gene profiles in multiple SCC cell lines to ES cell profiles and determined that SOX2 binds to distinct genomic loci in SCCs. In SCCs, SOX2 preferentially interacts with the transcription factor p63, as opposed to the transcription factor OCT4, which is the preferred SOX2 binding partner in ES cells. SOX2 and p63 exhibited overlapping genomic occupancy at a large number of loci in SCCs; however, coordinate binding of SOX2 and p63 was absent in ES cells. We further demonstrated that SOX2 and p63 jointly regulate gene expression, including the oncogene ETV4, which was essential for SOX2-amplified SCC cell survival. Together, these findings demonstrate that the action of SOX2 in SCC differs substantially from its role in pluripotency. The identification of the SCC-associated interaction between SOX2 and p63 will enable deeper characterization the downstream targets of this interaction in SCC and normal squamous epithelial physiology.

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Section: Figurementioning

confidence: 99%

SOX2 and p63 colocalize at genetic loci in squamous cell carcinomas

Watanabe¹,

Ma²,

Peng³

et al. 2014

J. Clin. Invest.

141

150

View full text Add to dashboard Cite

show abstract

“…Epithelial differentiation: Keratin 1 (KRT1) -KRT1 is a marker for terminal differentiation in the mammalian epidermis (Lessin et al, 1988;Huang et al, 2012). Through protein-protein interactions with other transcription and cofactors, TP63 also contributes to the transcriptional regulation of genes involved in cellular differentiation, proliferation/survival, growth suppression, apoptosis, adhesion, inflammation, and metabolism (Perez and Pietenpol, 2007;Viganò and Mantovani, 2007;Yang et al, 2011). Recent work by our laboratory has identified protein-protein interactions between ∆Np63α, TAp73, and c-REL that function to regulate key genes involved in growth arrest and apoptosis of mutant p53 head and neck squamous cell carcinoma (HNSCC) .…”

Section: Functionmentioning

confidence: 99%

“…Apoptosis: p53-Upregulated Modulator of Apoptosis (PUMA) -PUMA binds to BCL2 to induce rapid and profound apoptosis by cytochrome c release (Yu et al, 2001;Flores et al, 2002). Additionally, recent work has shown that a complex of ∆Np63α, with TAp73 or c-REL, can modify expression of key growth arrest and apoptotic genes such as p21WAF1, NOXA, and PUMA Yang et al, 2011). Adhesion: Integrin Alpha 6 (ITGA6) -ITGA6 is a cell surface adhesion molecule that may help regulate migration and layer formation, especially in epithelial cells.…”

Section: Functionmentioning

confidence: 99%

“…Mouse models deficient in ITGA6 display severe blistering of the skin and other epithelia and die shortly after birth (Georges-Labouesse et al, 1996;Carroll et al, 2006). Loss of endogenous p63 in mammary epithelial cells has been shown to induce detachment and cell death, presumably because p63 regulates expression of key adhesion molecules such as ITGA6, ITGB1, ITGB4 other ECM components, and cadherinscatenins (Carroll et al, 2006;Yang et al, 2011). Inflammation: ∆Np63 overexpression has been observed in head and neck squamous cell carcinoma (HNSCC), which are associated with inflammation.…”

Section: Functionmentioning

confidence: 99%

“…Inflammation: ∆Np63 overexpression has been observed in head and neck squamous cell carcinoma (HNSCC), which are associated with inflammation. TNF-α, a potent pro-inflammatory cytokine, promoted NF-κB, c-REL and RELA complexes with nuclear ∆Np63, to promote a broad-spectrum production of cytokines and chemokines Yang et al, 2011). In addition, in squamous epithelia of ∆Np63α transgenic mice, severe inflammation, skin lesions and erythema were observed after ∆Np63 expression was induced.…”

Section: Functionmentioning

confidence: 99%

See 2 more Smart Citations

TP63 (tumor protein p63)

Mattox¹,

Chen²,

Waes³

2013

Atlas of Genetics and Cytogenetics in Oncology and Haematology

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HSF1 activates the FOXO3a–ΔNp63α–CDK4 axis to promote head and neck squamous cell carcinoma cell proliferation and tumour growth

et al. 2023

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Head and neck squamous cell carcinoma (HNSCC) is one of the most prevalent cancers worldwide. Heat shock factor 1 (HSF1) is a conserved transcriptional factor that plays a critical role in maintaining cellular proteostasis. However, the role of HSF1 in HNSCC development remains largely unclear.Here, we report that HSF1 promotes forkhead box protein O3a (FOXO3a)dependent transcription of DNp63a (p63 isoform in the p53 family; inhibits cell migration, invasion, and metastasis), which leads to upregulation of cyclin-dependent kinase 4 expression and HNSCC tumour growth. Ablation of HSF1 or treatment with KRIBB11, a specific pharmacological inhibitor of HSF1, significantly suppresses DNp63a expression and HNSCC tumour growth. Clinically, the expression of HSF1 is positively correlated with the expression of DNp63a in HNSCC tumours. Together, this study demonstrates that the HSF1-DNp63a pathway is critically important for HNSCC tumour growth.

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ΔNp63 Versatilely Regulates a BroadNF-κBGene Program and Promotes Squamous Epithelial Proliferation, Migration, and Inflammation

Cited by 121 publications

References 46 publications

SOX2 and p63 colocalize at genetic loci in squamous cell carcinomas

SOX2 and p63 colocalize at genetic loci in squamous cell carcinomas

TP63 (tumor protein p63)

HSF1 activates the FOXO3a–ΔNp63α–CDK4 axis to promote head and neck squamous cell carcinoma cell proliferation and tumour growth

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