Switch from p53 to MDM2 as differentiating human keratinocytes lose their proliferative potential and increase in cellular size

Dazard, Jean-Eudes; Piette, Jacques; Basset-Séguin, Nicole; Blanchard, Jean Marie; Gandarillas, Alberto

doi:10.1038/sj.onc.1203695

Cited by 53 publications

(55 citation statements)

References 82 publications

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“…Induction of p21 during keratinocyte differentiation has been reported previously. 16,17,23,41 In our experiments, p21 was transiently induced in suspended keratinocytes and bound Cyclin A/cdk1 and Cyclin B/cdk1 at the time of the commitment to differentiation (6 h), whereas the binding to cdk2 peaked later on. Interestingly, p21 is required for the downregulation of Cyclin A in mouse keratinocytes.…”

Section: Discussionmentioning

confidence: 96%

Cyclin E drives human keratinocyte growth into differentiation

et al. 2012

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Human epidermis is continuously exposed to environmental mutagenic hazard and is the most frequent target of human cancer. How the epidermis coordinates proliferation with differentiation to maintain homeostasis, even in hyperproliferative conditions, is unclear. For instance, overactivation of the proto-oncogene MYC in keratinocytes stimulates differentiation. Here we explore the cell cycle regulation as proliferating human keratinocytes commit to terminal differentiation upon loss of anchorage or overactivation of MYC. The S-phase of the cell cycle is deregulated as mitotic regulators are inhibited in the onset of differentiation. Experimental inhibition of mitotic kinase cdk1 or kinases of the mitosis spindle checkpoint Aurora B or Pololike Kinase, triggered keratinocyte terminal differentiation. Furthermore, hyperactivation of the cell cycle by overexpressing the DNA replication regulator Cyclin E induced mitosis failure and differentiation. Inhibition of Cyclin E by shRNAs attenuated the induction of differentiation by MYC. In addition, we present evidence that Cyclin E induces DNA damage and the p53 pathway. The results provide novel clues for the mechanisms committing proliferative keratinocytes to differentiate, with implications for tissue homeostasis maintenance, HPV amplification and tumorigenesis.

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Section: Discussionmentioning

confidence: 96%

Cyclin E drives human keratinocyte growth into differentiation

et al. 2012

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“…Thus, p21 may provide a means of evading apoptosis, during the transition between differentiated states, as shown in several systems (Poluha et al, 1996;Wang and Walsh, 1996;Lawlor and Rotwein, 2000). Moreover, keratinocyte differentiation is accompanied by induction of mdm2 and concomitant downmodulation of p53 activity and, interestingly, is coincident with increased cell size and ploidy (Dazard et al, 2000). However, in the mammary gland, overexpression of mdm2 generated polyploid cells irrespective of p53 status, suggesting additional p53-independent roles for mdm2 in the regulation of DNA synthesis (Lundgren et al, 1997).…”

Section: Cytokinesis Failure and Polyploid Progression Predispose Tramentioning

confidence: 99%

p53 deficiency exacerbates pleiotropic mitotic defects, changes in nuclearity and polyploidy in transdifferentiating pancreatic acinar cells

Sphyris

Harrison

2005

Oncogene

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In a primary culture model for pancreatic acinar-ductal transdifferentiation, cells exhibited increased proliferation, changes in nuclearity and polyploidy. We identify the 'nucleus to centrosome' ratio of the progenitor cell, the dissemination of centrosomes at spindle poles and cytokinesis failure as critical determinants of mitosis outcome and centrosome inheritance. Abortive cytokinesis of mononuclear cells contributes to the binuclear cell pool, whereas enclosure of entire mitotic formations, within a single nuclear envelope, perpetuates polyploidization. Binuclear cell nuclei combine their genomes on a single metaphase plate, doubling descendant ploidy. Moreover, B42% of binuclear and tetraploid cells assemble aberrant spindles with up to 8 centrosomes/poles. These phenotypes were exacerbated in p53-deficient cultures exhibiting increased S-phase entry, giant nuclei, multinucleation, multipolar mitoses and centrosome hyperamplification. The tendency of p53-proficient cells to spontaneously evade the tetraploidy checkpoint degenerates to uncontrolled polyploid progression in p53-deficient cultures, explaining why p53 abrogation alone rapidly descends to aneuploidy in this system. We detected constitutively nuclear mdm2, which may circumvent endogenous cellcycle checkpoints, and pronounced accumulation of p21 and p27 in multinuclear cells and giant nuclei, consistent with roles in polyploidization. This in vitro model may recapitulate the processes underlying genomic instability in pancreatic tumours in vivo, and attests to the existence of a p53-dependent polyploidy checkpoint acting to limit the degree of polyploidization.

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“…Total cell lysates, protein resolution by PAGE, transfer on nitrocellulose membrane (Bio-Rad), and immunoblotting were performed as previously described (Dazard et al, 2000). Detection was performed using the Western blotting-enhanced chemiluminescence substrate (ECL þ plus, Amersham Pharmacia Biotech, Buckinghamshire, England) following the supplier's protocol.…”

Section: Antibodies and Immunoblot Analysismentioning

confidence: 99%

“…Fixation and staining were performed as previously described (Dazard et al, 2000). All cells were resuspended and filtered through a 70 mm mesh prior to analysis by flow cytometry on a Becton Dickinson FACScan s .…”

Section: Flow Cytometrymentioning

confidence: 99%

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Genome-wide comparison of human keratinocyte and squamous cell carcinoma responses to UVB irradiation: implications for skin and epithelial cancer

et al. 2003

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To gain insight into the transformation of epidermal cells into squamous carcinoma cells (SCC), we compared the response to ultraviolet B radiation (UVB) of normal human epidermal keratinocytes (NHEK) versus their transformed counterpart, SCC, using biological and molecular profiling. DNA microarray analyses (Affymetrix s , B12 000 genes) indicated that the major group of upregulated genes in keratinocytes fall into three categories: (i) antiapoptotic and cell survival factors, including chemokines of the CXC/CC subfamilies (e.g. IL-8, GRO-1, -2, -3, SCYA20), growth factors (e.g. HB-EGF, CTGF, INSL-4), and proinflammatory mediators (e.g. COX-2, S100A9), (ii) DNA repair-related genes (e.g. GADD45, ERCC, BTG-1, Histones), and (iii) ECM proteases (MMP-1, -10). The major downregulated genes are DNp63 and PUMILIO, two potential markers for the maintenance of keratinocyte stem cells. NHEK were found to be more resistant than SCC to UVB-induced apoptosis and this resistance was mainly because of the protection from cell death by secreted survival factors, since it can be transferred from NHEK to SCC cultures by the conditioned medium. Whereas the response of keratinocytes to UVB involved regulation of key checkpoint genes (p53, MDM2, p21 Cip1 , DNp63), as well as antiapoptotic and DNA repair-related genes -no or little regulation of these genes was observed in SCC. The effect of UVB on NHEK and SCC resulted in upregulation of 251 and 127 genes, respectively, and downregulation of 322 genes in NHEK and 117 genes in SCC. To further analyse these changes, we used a novel unsupervised coupled two-way clustering method that allowed the identification of groups of genes that clearly partitioned keratinocytes from SCC, including a group of genes whose constitutive expression levels were similar before UVB. This allowed the identification of discriminating genes not otherwise revealed by simple static comparison in the absence of UVB irradiation. The implication of the changes in gene profile in keratinocytes for epithelial cancer is discussed.

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Switch from p53 to MDM2 as differentiating human keratinocytes lose their proliferative potential and increase in cellular size

Cited by 53 publications

References 82 publications

Cyclin E drives human keratinocyte growth into differentiation

Cyclin E drives human keratinocyte growth into differentiation

p53 deficiency exacerbates pleiotropic mitotic defects, changes in nuclearity and polyploidy in transdifferentiating pancreatic acinar cells

Genome-wide comparison of human keratinocyte and squamous cell carcinoma responses to UVB irradiation: implications for skin and epithelial cancer

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