Skin human papillomavirus type 38 alters p53 functions by accumulation of ΔNp73

Accardi, Rosita; Dong, Wen; Smet, Anouk; R, Cui; Hautefeuille, A.; Gabet, Anne Sophie; Sylla, Bakary S.; Gissmann, Lutz; Hainaut, Pierre; Tommasino, Massimo

doi:10.1038/sj.embor.7400615

Cited by 102 publications

(147 citation statements)

References 16 publications

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“…We therefore determined whether similar events occurred in the mouse model. DNp73 expression levels were analysed by reverse transcriptase-PCR in HPV38 E6/E7 Tg mice in the presence or absence of p53 as previously described (Accardi et al, 2006). In agreement with the in vitro data, we observed that p53 À/À HPV38 E6/E7 Tg mice did not express DNp73 (Figure 1a).…”

supporting

confidence: 76%

“…Since downregulation of DNp73 by antisense oligonucleotide in HPV38 E6/E7 keratinocytes led to a restoration of p53 transcriptional functions (Accardi et al, 2006), we next determined whether similar events can occur in HPV38 E6/E7 Tg mice lacking DNp73. HPV38 E6/E7 Tg mice were crossed with p73 À/À mice, which were previously generated by replacing the exons 5 and 6, leading to deficiency of all p73 isoforms (Yang et al, 2000).…”

mentioning

confidence: 99%

“…In fact, while HPV16 E6 induces p53 degradation via the proteasome pathway (zur Hausen, 2002), HPV38 E6 and E7 promote the accumulation of a specific p53 form that selectively activates the transcription of DNp73, which in turn inhibits p53 ability to induce the transcription of genes involved in growth suppression and apoptosis (Accardi et al, 2006). The accumulation of p53 and DNp73 was also detected in keratinocytes of transgenic (Tg) mice expressing HPV38 E6 and E7 under the control of keratin-10 promoter (Accardi et al, 2006). In addition, in contrast to normal mice, HPV38 E6/E7 Tg mice do not respond to ultraviolet (UV) irradiation.…”

mentioning

confidence: 99%

“…Characterization of the biological properties of the products of the early genes E6 and E7 from different beta HPV types in in vitro and in vivo model has highlighted the potential carcinogenicity of these viruses (Jackson et al, 2000;Caldeira et al, 2003;Akgul et al, 2005;Dong et al, 2005;Schaper et al, 2005;Accardi et al, 2006;Michel et al, 2006). We showed that expression of E6 and E7 from the beta HPV38 in primary human keratinocytes results in inactivation of the tumour suppressor p53 and pRb and immortalization (Caldeira et al, 2003;Accardi et al, 2006). Interestingly, HPV38 inactivates p53 functions by a mechanism that differs from the one used by the mucosal high-risk HPV16.…”

mentioning

confidence: 99%

“…To evaluate this hypothesis, we have crossed HPV38 E6/E7 Tg mice with p53 null mice (Donehower et al, 1992). Identification of the different Tg lines was achieved by extracting DNA from the tails of 5-week-old mice followed by PCR with specific primers for the K10 HPV38 E6 and E7 region and p53 In vitro experiments in primary human keratinocytes showed that p53 gene silencing by small interfering RNA abolished DNp73 transcription activation (Accardi et al, 2006). We therefore determined whether similar events occurred in the mouse model.…”

mentioning

confidence: 99%

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Loss of p53 or p73 in human papillomavirus type 38 E6 and E7 transgenic mice partially restores the UV-activated cell cycle checkpoints

et al. 2007

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We have previously shown that human keratinocytes expressing E6 and E7 from the cutaneous human papillomavirus (HPV) type 38 have high levels of a specific form of p53, which in turn activate the transcription of DNp73 gene. Expression of HPV38 E6 and E7 in mouse skin also promotes p53 and DNp73 accumulation. Interestingly, keratinocytes of these mice do not undergo cell cycle arrest after skin ultraviolet (UV) irradiation. Here, we provide several lines of evidence that DNp73 expression and lack of the UV response are directly linked. Loss of p53 gene in HPV38 E6/E7 transgenic mice abolished DNp73 expression and partially restored the UV-activated cell cycle checkpoints. Similarly, loss of p73, and consequently DNp73, led to restoration of the p53 pathways. In fact, keratinocytes of p73 À/À HPV38 E6/E7 transgenic mice upon UV irradiation express high levels of p21 WAF1 and are cell cycle arrested. Thus, HPV38 E6 and E7, via DNp73 accumulation, are able to alter the regulation of cell cycle checkpoints activated by UV radiation. These data suggest that UV and HPV may cooperate in skin carcinogenesis.

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supporting

confidence: 76%

mentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Loss of p53 or p73 in human papillomavirus type 38 E6 and E7 transgenic mice partially restores the UV-activated cell cycle checkpoints

et al. 2007

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Skin Cancer in the Immunocompromised Patient

Harwood

McGregor

Proby³

2016

Rook's Textbook of Dermatology, Ninth Edition

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The immune system plays a critical role in skin cancer development, progression and destruction. Skin cancers in individuals with compromised immune systems represent a growing challenge in terms of their frequency and diversity as well as their atypical and often aggressive nature. Mortality and morbidity associated with skin tumours in this clinical context are often considerable, their pathogenesis is multifactorial and an evidence base to guide management is lacking in many key areas.

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Risk of squamous cell skin cancer after organ transplant associated with antibodies to cutaneous papillomaviruses, polyomaviruses, and TMC6/8 (EVER1/2) variants

et al. 2014

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Squamous cell skin cancer (SCSC) disproportionately affects organ transplant recipients, and may be related to increased viral replication in the setting of immune suppression. We conducted a nested case–control study among transplant recipients to determine whether SCSC is associated with antibodies to cutaneous human papillomaviruses (HPV), to genes associated with a rare genetic susceptibility to HPV (TMC6/TMC8), or to human polyomaviruses (HPyV). Cases (n = 149) had histologically confirmed SCSC, and controls (n = 290) were individually matched to cases on time since transplant, type of transplant, gender, and race. All subjects had serum drawn immediately prior to transplant surgery. Antibodies to 25 cutaneous HPVs and six HPyVs were assayed by detection of binding to virus-like particles, and 11 TMC6/8 variants were genotyped. After correction for multiple comparisons, only antibodies to HPV37 were associated with SCSC (OR 2.0, 95% CI 1.2–3.4). Common genetic variants of TMC6/8 were not associated with SCSC, but three variants in TMC8 (rs12452890, rs412611, and rs7208422) were associated with greater seropositivity for species 2 betapapillomaviruses among controls. This study suggests that some betaHPVs, but not polyomaviruses, may play a role in the excess risk of SCSC among transplant recipients.

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Skin human papillomavirus type 38 alters p53 functions by accumulation of ΔNp73

Cited by 102 publications

References 16 publications

Loss of p53 or p73 in human papillomavirus type 38 E6 and E7 transgenic mice partially restores the UV-activated cell cycle checkpoints

Loss of p53 or p73 in human papillomavirus type 38 E6 and E7 transgenic mice partially restores the UV-activated cell cycle checkpoints

Skin Cancer in the Immunocompromised Patient

Risk of squamous cell skin cancer after organ transplant associated with antibodies to cutaneous papillomaviruses, polyomaviruses, and TMC6/8 (EVER1/2) variants

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