UVB-induced mutations in human key gatekeeper genes governing signalling pathways and consequences for skin tumourigenesis

Ehrhart, Jean-Claude; Gosselet, Fabien; Culerrier, Raphaël; Sarasin, Alain

doi:10.1039/b302281a

Cited by 46 publications

(29 citation statements)

References 67 publications

(97 reference statements)

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“…Its activation and accumulation is triggered by a variety of stress signals, which relies on an autoregulatory loop. In fact, it is well known that after the stress signalling, the p53 protein becomes more stable and accumulates (Ehrhart et al, 2003). The UVC-p53 modulation found in XP/CS is the first observation of transcriptional regulation of this protein after a stress situation in DNA repair-deficient cells.…”

Section: Uvc Transcript Modulation In Xp/cs Cellsmentioning

confidence: 95%

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Transcriptional profiles of unirradiated or UV-irradiated human cells expressing either the cancer-prone XPB/CS allele or the noncancer-prone XPB/TTD allele

et al. 2004

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Section: Uvc Transcript Modulation In Xp/cs Cellsmentioning

confidence: 95%

“…Cyclin D1 has an important role in the progression of cell cycle. It associates with cyclin-dependent kinases (CDK) CDK4 and CDK6 to phosphorylate the pRB protein during the G1 phase (Ehrhart et al, 2003).…”

Section: Uvc Modulation Of the Ttd Cell Transcriptomementioning

confidence: 99%

Transcriptional profiles of unirradiated or UV-irradiated human cells expressing either the cancer-prone XPB/CS allele or the noncancer-prone XPB/TTD allele

et al. 2004

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“…Female breeders (6)(7) weeks old) of p53 -/-/ C57BL/6J strain were purchased from the Jackson Laboratory and were acclimatized for 1 week before being recruited to breeding. The male breeders of SKH-1 hairless strain (5-6 weeks old) were purchased from Charles River Laboratories and also acclimatized for a week as described earlier.…”

Section: Skh-1 Hairless Mice Female Skh-1 Hairless Mice (4-6 Weeks Old)mentioning

confidence: 99%

“…p53 mutations occur in the majority of SCCs, basal cell carcinomas, actinic keratoses, and perilesional nontumor skin adjacent to these lesions. These mutations are detectable early in the development of UVB-induced NMSCs (7,8). In murine models, UVB-associated p53 gene mutations also contribute to tumor development and are C to T and CC to TT transitions at dipyrimidine sites.…”

Section: Introductionmentioning

confidence: 99%

CP-31398 restores mutant p53 tumor suppressor function and inhibits UVB-induced skin carcinogenesis in mice

Tang

Zhu²,

Han³

et al. 2007

J. Clin. Invest.

116

100

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Mutations in the tumor suppressor p53 are detectable in over 50% of all human malignancies. Mutant p53 protein is incapable of transactivating its downstream target genes that are required for DNA repair and apoptosis. Chronic exposure to UVB induces p53 mutations and is carcinogenic in both murine and human skin. CP-31398, a styrylquinazoline compound, restores the tumor suppressor functions of mutant forms of p53 in tumor cells. However, its effectiveness in vivo remains unclear. Here, we demonstrate that CP-31398 blocked UVB-induced skin carcinogenesis and was associated with increases in p53, p21, and BclXs. CP-31398 downregulated Bcl2, proliferating nuclear cell antigen, and cyclin D1. Activation of caspase-3 and cleavage of poly (ADP-ribose) polymerase also occurred in both tumor and perilesional skin following treatment. CP-31398 induced the expression of p53-dependent target proteins, and this was followed by apoptosis in UVB-irradiated wild-type mice but not in their p53-deficient littermates. Similar effects were observed in human skin carcinoma A431 cells expressing mutant p53. In addition, CP-31398 induced mitochondrial translocation of p53, leading to changes in mitochondrial membrane permeability pore transition (MPT) and consequent cytochrome c release in these cells. Blocking MPT diminished p53 translocation and apoptosis. These studies indicate that reconstituting p53 tumor suppressor functions in vivo by small molecular weight compounds may block the pathogenesis and progression of skin cancer.

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“…25 In the above example, a possible explanation is that GK protein overexpression may be not only tolerated but also selected in the presence of a block affecting heterologous TSGs. 26,27 Consistent with this, CT inactivation is a common tumorigenetic event predisposing to GK mutation; 28 for example, repair deficiency (for example, microsatellite instability caused by mismatch repair gene inactivation) may lead to secondary mutations (for example, frameshifts) affecting GKs or POs in preinvasive tissues. 29,30 Moreover, as repair genes are involved in afferent sensing of DNA damage, 31,32 CT inactivation in tumors could also bias GK function towards a pro-mitogenic phenotype by raising the apoptotic threshold.…”

Section: Introductionmentioning

confidence: 86%

Unexpected functional similarities between gatekeeper tumour suppressor genes and proto-oncogenes revealed by systems biology

Zhao

Epstein

2011

J Hum Genet

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Familial tumor suppressor genes comprise two subgroups: caretaker genes (CTs) that repair DNA, and gatekeeper genes (GKs) that trigger cell death. Since GKs may also induce cell cycle delay and thus enhance cell survival by facilitating DNA repair, we hypothesized that the prosurvival phenotype of GKs could be selected during cancer progression, and we used a multivariable systems biology approach to test this. We performed multidimensional data analysis, non-negative matrix factorization and logistic regression to compare the features of GKs with those of their putative antagonists, the proto-oncogenes (POs), as well as with control groups of CTs and functionally unrelated congenital heart disease genes (HDs). GKs and POs closely resemble each other, but not CTs or HDs, in terms of gene structure (Po0.001), expression level and breadth (Po0.01), DNA methylation signature (Po0.001) and evolutionary rate (Po0.001). The similar selection pressures and epigenetic trajectories of GKs and POs so implied suggest a common functional attribute that is strongly negatively selected-that is, a shared phenotype that enhances cell survival. The counterintuitive finding of similar evolutionary pressures affecting GKs and POs raises an intriguing possibility: namely, that cancer microevolution is accelerated by an epistatic cascade in which upstream suppressor gene defects subvert the normal bifunctionality of wild-type GKs by constitutively shifting the phenotype away from apoptosis towards survival. If correct, this interpretation would explain the hitherto unexplained phenomenon of frequent wild-type GK (for example, p53) overexpression in tumors.

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UVB-induced mutations in human key gatekeeper genes governing signalling pathways and consequences for skin tumourigenesis

Cited by 46 publications

References 67 publications

Transcriptional profiles of unirradiated or UV-irradiated human cells expressing either the cancer-prone XPB/CS allele or the noncancer-prone XPB/TTD allele

Transcriptional profiles of unirradiated or UV-irradiated human cells expressing either the cancer-prone XPB/CS allele or the noncancer-prone XPB/TTD allele

CP-31398 restores mutant p53 tumor suppressor function and inhibits UVB-induced skin carcinogenesis in mice

Unexpected functional similarities between gatekeeper tumour suppressor genes and proto-oncogenes revealed by systems biology

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