FGF8, c-Abl and p300 participate in a pathway that controls stability and function of the ΔNp63<i>α</i>protein

Restelli, Michela; Molinari, Elisa; Marinari, Barbara; Conte, Daniele; Gnesutta, Nerina; Costanzo, Antonio; Merlo, Giorgio R.; Guerrini, Luisa

doi:10.1093/hmg/ddv151

Cited by 12 publications

(18 citation statements)

References 56 publications

(98 reference statements)

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“…This is supported by the SHFM observed in Dlx2/5 −/− mice (Figure ) . The split hindlimbs in Dlx5/6 −/− mice are the result of a cell‐autonomous failure of the central AER to regulate p63 and to maintain and express morphogenetic signals (Figure ) . The degeneration of the AER in Dlx5/6 −/− mice led to SHFM phenotype which is similar to the phenotype of Dactylaplasia mice .…”

Section: Shfm‐associated Genesmentioning

confidence: 89%

“…Fgf8 functions are to sustain epithelial‐mesenchymal signaling and assure the timely generation of the correct population of mesenchymal progenitors . It in turn regulates the function and stability of ΔNp63α by increasing the binding of ΔNp63α to the tyrosine kinase c‐Abl and the level of ΔNp63α acetylation . Aberration of Fgf8 expression is hypothesized to cause malfunction of ΔNp63α (Figure ).…”

Section: Shfm‐associated Genesmentioning

confidence: 99%

Section: Shfm‐associated Genesmentioning

confidence: 99%

“…45 It in turn regulates the function and stability of ΔNp63α by increasing the binding of ΔNp63α to the tyrosine kinase c-Abl and the level of ΔNp63α acetylation. 25 Aberration of Fgf8 expression is hypothesized to cause malfunction of ΔNp63α (Figure 2). In order for a normal limb to develop, Fgf8 is crucial for the correct establishment of the signaling loop within the developing limb bud.…”

Section: Zak and Shfmmentioning

confidence: 99%

“…In order for mice to have SHFM, alterations in Fgf8 expression need to accompany abnormal expression of other genes in AER as well. Loss of Fgf8 or mutations in Fgf8 leads to abnormal ΔNp63α protein stability,24,25,44 failure of AER stratification, and subsequent aberrant limb development (Figure 2) 45. All lines of evidence suggest that abnormalities of TP63, WNT10B, DLX5, DLX6, FGF8, and FGFR1 lead to dysregulation of FGF8 in the central portion of the AER and subsequently lead to misexpression of a number of AER genes, failure of its stratification, and thus SHFM (Figure 2).…”

mentioning

confidence: 99%

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Genetic regulatory pathways of split‐hand/foot malformation

Kantaputra

Carlson

2018

Clinical Genetics

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Split-hand/foot malformation (SHFM) is caused by mutations in TP63, DLX5, DLX6, FGF8, FGFR1, WNT10B, and BHLHA9. The clinical features of SHFM caused by mutations of these genes are not distinguishable. This implies that in normal situations these SHFM-associated genes share an underlying regulatory pathway that is involved in the development of the central parts of the hands and feet. The mutations in SHFM-related genes lead to dysregulation of Fgf8 in the central portion of the apical ectodermal ridge (AER) and subsequently lead to misexpression of a number of downstream target genes, failure of stratification of the AER, and thus SHFM. Syndactyly of the remaining digits is most likely the effects of dysregulation of Fgf-Bmp-Msx signaling on apoptotic cell death. Loss of digit identity in SHFM is hypothesized to be the effects of misexpression of HOX genes, abnormal SHH gradient, or the loss of balance between GLI3A and GLI3R. Disruption of canonical and non-canonical Wnt signaling is involved in the pathogenesis of SHFM. Whatever the causative genes of SHFM are, the mutations seem to lead to dysregulation of Fgf8 in AER cells of the central parts of the hands and feet and disruption of Wnt-Bmp-Fgf signaling pathways in AER.

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Section: Shfm‐associated Genesmentioning

confidence: 89%

Section: Shfm‐associated Genesmentioning

confidence: 99%

Section: Shfm‐associated Genesmentioning

confidence: 99%

Section: Zak and Shfmmentioning

confidence: 99%

mentioning

confidence: 99%

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Genetic regulatory pathways of split‐hand/foot malformation

Kantaputra

Carlson

2018

Clinical Genetics

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The foggy world(s) of p63 isoform regulation in normal cells and cancer

Pokorná

Vysloužil

Hrabal

et al. 2021

The Journal of Pathology

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The p53 family member p63 exists as two major protein variants (TAp63 and ΔNp63) with distinct expression patterns and functional properties. Whilst downstream target genes of p63 have been studied intensively, how p63 variants are themselves controlled has been relatively neglected. Here, we review advances in understanding ΔNp63 and TAp63 regulation, highlighting their distinct pathways. TAp63 has roles in senescence and metabolism, and in germ cell genome maintenance, where it is activated post‐transcriptionally by phosphorylation cascades after DNA damage. The function and regulation of TAp63 in mesenchymal and haematopoietic cells is less clear but may involve epigenetic control through DNA methylation. ΔNp63 functions to maintain stem/progenitor cells in various epithelia and is overexpressed in squamous and certain other cancers. ΔNp63 is transcriptionally regulated through multiple enhancers in concert with chromatin modifying proteins. Many signalling pathways including growth factors, morphogens, inflammation, and the extracellular matrix influence ΔNp63 levels, with inconsistent results reported. There is also evidence for reciprocal regulation, including ΔNp63 activating its own transcription. ΔNp63 is downregulated during cell differentiation through transcriptional regulation, while post‐transcriptional events cause proteasomal degradation. Throughout the review, we identify knowledge gaps and highlight discordances, providing potential explanations including cell‐context and cell–matrix interactions. Identifying individual p63 variants has roles in differential diagnosis and prognosis, and understanding their regulation suggests clinically approved agents for targeting p63 that may be useful combination therapies for selected cancer patients. © 2021 The Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

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TP63 links chromatin remodeling and enhancer reprogramming to epidermal differentiation and squamous cell carcinoma development

Man

Tan

Wang

et al. 2020

Cell. Mol. Life Sci.

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Squamous cell carcinoma (SCC) is an aggressive malignancy that can originate from various organs. TP63 is a master regulator that plays an essential role in epidermal differentiation. It is also a lineage-dependent oncogene in SCC. ΔNp63α is the prominent isoform of TP63 expressed in epidermal cells and SCC, and overexpression promotes SCC development through a variety of mechanisms. Recently, ΔNp63α was highlighted to act as an epidermal-specific pioneer factor that binds closed chromatin and enhances chromatin accessibility at epidermal enhancers. ΔNp63α coordinates chromatin-remodeling enzymes to orchestrate the tissue-specific enhancer landscape and three-dimensional high-order architecture of chromatin. Moreover, ΔNp63α establishes squamous-like enhancer landscapes to drive oncogenic target expression during SCC development. Importantly, ΔNp63α acts as an upstream regulator of super enhancers to activate a number of oncogenic transcripts linked to poor prognosis in SCC. Mechanistically, ΔNp63α activates genes transcription through physically interacting with a number of epigenetic modulators to establish enhancers and enhance chromatin accessibility. In contrast, ΔNp63α also represses gene transcription via interacting with repressive epigenetic regulators. ΔNp63α expression is regulated at multiple levels, including transcriptional, post-transcriptional, and post-translational levels. In this review, we summarize recent advances of p63 in epigenomic and transcriptional control, as well as the mechanistic regulation of p63.

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FGF8, c-Abl and p300 participate in a pathway that controls stability and function of the ΔNp63αprotein

Cited by 12 publications

References 56 publications

Genetic regulatory pathways of split‐hand/foot malformation

Genetic regulatory pathways of split‐hand/foot malformation

The foggy world(s) of p63 isoform regulation in normal cells and cancer

TP63 links chromatin remodeling and enhancer reprogramming to epidermal differentiation and squamous cell carcinoma development

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