Role of HPV E6 proteins in preventing UVB-induced release of pro-apoptotic factors from the mitochondria

Leverrier, Sabrina; Bergamaschi, Daniele; Ghali, Lucy; Ola, Ayodele; Warnes, Gary; Akgül, Baki; Blight, Ken; García‐Escudero, Ramón; Penna, Aubin; Eddaoudi, Ayad; Storey, Alan

doi:10.1007/s10495-006-0004-1

Cited by 73 publications

(76 citation statements)

References 46 publications

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“…Cell lines stably expressing HPV5 E6-HA mutants (derived from HT1080) were UVB irradiated at 1 m J cm 22 and harvested after 24 hr as described. Apoptosis assay cells were removed using trypsin and handled on ice.…”

Section: Flow Cytometrymentioning

confidence: 99%

“…21 We have previously shown that the HPV E6 protein of b-HPV types targets Bak for ubiquitin mediated degradation, 7 an E6 activity that prevents release of proapoptotic mitochondrial factors thereby maintaining mitochondrial integrity and function. 22 In marked difference to anogenital HPVs, b-type viruses such as HPV8 do not target p53 for proteolysis and do not interact with the E6-AP ubiquitin ligase utilized by anogenital HPV E6 proteins to signal p53 destruction. 23 Analysis of NMSC biopsies has also revealed that HPVnegative tumours have both a high apoptotic and proliferation rate compared to HPV-positive tumours that are also highly proliferative, but in contrast have a low apoptotic rate, in addition to significantly reduced levels of Bak.…”

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confidence: 99%

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Identification of the regions of the HPV 5 E6 protein involved in Bak degradation and inhibition of apoptosis

Simmonds

Storey

2008

Intl Journal of Cancer

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UVB induced DNA damage is the major aetiological agent in NMSC development, but mounting evidence suggests a role for human papillomaviruses (HPV) from genus beta, including HPV 5 and HPV 8, in the development of NMSC on sun exposed body sites. We have previously shown that UVB activates Bak, an apoptogenic mitochondrial factor that, following an apoptotic stimulus, undergoes a conformational change that leads to pore formation in the mitochondrial membrane that releases apoptotic factors. The HPV E6 protein effectively inhibits UVB-induced apoptosis and targets Bak for proteolytic degradation. We have now identified the regions of the HPV5 E6 that are required to mediate Bak proteolysis and contribute toward the antiapoptotic activity of the protein. Interestingly, while wild-type HPV5 E6 does not bind or target p53 for proteolysis, we have isolated specific HPV5 E6 mutants that switch target specificity from Bak to p53 in a p53 codon 72 isoform-dependent manner. Furthermore, we demonstrate that the ability of wild-type HPV5 E6 to target Bak or specific E6 mutants to target p53 for proteolysis is not dependent on the E6-AP ubiquitin ligase. ' 2008 Wiley-Liss, Inc.Key words: skin cancer; HPV; Bak; E6; UV; light Chronic exposure to solar UV irradiation has been identified as the primary causative agent in the development of nonmelanoma skin cancer (NMSC).1 The formation of ''sunburn cells'' frequently observed in epidermis treated with UVB display apoptotic characteristic such as condensed nuclei, 2,3 and the response to UVB radiation is in part dependent upon the expression of p53. 4This p53-driven response, often termed ''cellular proofreading'', eliminates rather than repairs severely damaged cells, however p53-independent pathways have also been described. [5][6][7] However, studies indicate that Li Fraumeni patients, who have only one copy of p53, and patients with regions of mutated p53 on sunexposed sites, are not predisposed to tumour development 8,9 indicating that p53-independent mechanisms also play an important role in eliminating damaged cells.Studies on Epidermodysplasia Verruciformis (EV) patients have identified a link between extensive wart infection and the development of skin tumours on sun-exposed sites.10 Epidemiological studies also invoke a role for HPV in NMSC development in both immunocompromised organ transplant recipients and immunocompetent individuals. 11,12 There is increasing evidence that b-HPV types facilitate the persistence of DNA-damaged cells within the epithelium, following UVB-exposure, chiefly through interfering with DNA damage responses and inhibiting apoptotic pathways, reviewed by Akg€ ul et al. 13The Bak protein is a key apoptogenic factor located in the outer mitochondrial membrane.14 Following UV exposure, Bak is activated and stabilized in a p53-independent manner 7 by BH3 domain-containing proteins. 15,16 Bak activation involves a change in conformation at the N-terminus of the prote in 17 leading to Bak multimerization, [18][19][20] that is believed to form pores...

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Section: Flow Cytometrymentioning

confidence: 99%

mentioning

confidence: 99%

Identification of the regions of the HPV 5 E6 protein involved in Bak degradation and inhibition of apoptosis

Simmonds

Storey

2008

Intl Journal of Cancer

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“…In addition, functional inactivation of p53 through activation of DNp73a has been detected in HPV38 E6E7-expressing human keratinocytes (Accardi et al, 2006). As the vast majority of SCCs are found on frequently UV-exposed skin and cumulative sun exposure is the most important known environmental SCC risk factor, the observation that HPV5 E6 eliminated UVBinduced apoptosis via degradation of Bak, thereby inhibiting the release of apoptosis-inducing factor, is particularly interesting Leverrier et al, 2007). This suggests that UV radiation-induced genotoxic DNA damage is potentially facilitated by bPVs (Bouwes Bavinck & Feltkamp, 2004).…”

Section: Introductionmentioning

confidence: 99%

Specific betapapillomaviruses associated with squamous cell carcinoma of the skin inhibit UVB-induced apoptosis of primary human keratinocytes

Struijk

Meijden

Kazem

et al. 2008

Journal of General Virology

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Epidemiological studies have shown an association between infections by specific betapapillomaviruses, such as human papillomavirus (HPV) types 5 and 8, and cutaneous squamous cell carcinoma (SCC). The role of betapapillomaviruses in the development of cutaneous SCC is, however, still enigmatic. The ability to inhibit UVB-induced apoptosis, as demonstrated for HPV5 in vitro, may be important in this respect, as survival of DNA-damaged and mutated cells increases the risk of transformation. The aim of this study was to assess whether inhibition of UVB-induced apoptosis is a general property of betapapillomaviruses and to identify apoptotic factors that are potentially involved in this process. Primary human keratinocytes transduced with E6 and E7 of selected betapapillomaviruses (HPV5, HPV8, HPV15, HPV20, HPV24 and HPV38) were characterized and subjected to UVB irradiation. HPV8-and HPV20-expressing keratinocytes in particular showed fewer signs of apoptosis, as demonstrated by lower levels of active caspase 3, less enzymic caspase activity and less DNA fragmentation. The observed inhibition of UVB-induced apoptosis was mediated by E6 and coincided with reduced steady-state expression of the pro-apoptotic protein Bax. In conclusion, E6 of HPV8 and HPV20 reduces the apoptotic responses upon UVB irradiation when expressed in primary human keratinocytes. Infections with HPV8 and HPV20 may therefore augment the carcinogenic effect of UV radiation and potentially contribute to oncogenic transformation of the skin.

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“…Actinic keratosis is regarded as an early precancerous intraepidermal neoplasia, which represents the cutaneous counterpart of squamous intraepithelial lesions in the genital mucosa. Interestingly, the high prevalence and viral load of bPV types in these precancerous skin lesions Weissenborn et al, 2005) and the decrease in viral load during skin carcinogenesis may point to a particular involvement of HPV in the early stages of skin cancer development.Recent publications have demonstrated that bHPV-expressing keratinocytes can potentially facilitate UV radiationinduced DNA damage, as they are able to inhibit apoptosis in response to UV damage (Jackson & Storey, 2000;Leverrier et al, 2007;Struijk et al, 2008;Underbrink et al, 2008) and compromise the repair of UV-induced DNA mutations (Giampieri & Storey, 2004). These mechanisms may lead to the persistence of UV-damaged keratinocytes.…”

mentioning

confidence: 99%

“…Recent publications have demonstrated that bHPV-expressing keratinocytes can potentially facilitate UV radiationinduced DNA damage, as they are able to inhibit apoptosis in response to UV damage (Jackson & Storey, 2000;Leverrier et al, 2007;Struijk et al, 2008;Underbrink et al, 2008) and compromise the repair of UV-induced DNA mutations (Giampieri & Storey, 2004). These mechanisms may lead to the persistence of UV-damaged keratinocytes.…”

mentioning

confidence: 99%

Human papillomavirus 5 and 8 E6 downregulate interleukin-8 secretion in primary human keratinocytes

Akgül

Bostancı

Westphal

et al. 2009

Journal of General Virology

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Human papillomaviruses (HPVs) of the genus Betapapillomavirus appear to be involved in the early stages of skin cancer development, since both the prevalence and viral load are higher in precancerous actinic keratoses than in skin cancers. is an inflammatory cytokine that serves to alert the surrounding tissue after UV-induced damage. We examined the effects of the E2, E6 and E7 proteins of HPV8 and the E6 proteins of various HPV genotypes on IL-8 secretion from primary keratinocytes. HPV5 and HPV8 E6 showed the highest downregulation of basal IL-8 secretion. HPV8 E6 also negatively modulated IL-8 mRNA expression and protein secretion upon UVB irradiation. The downregulation of IL-8 in actinic keratoses may weaken the response to UV-induced damage and thus favour the accumulation of UVB-induced mutations.Human papillomaviruses (HPVs) are small, doublestranded DNA viruses that infect keratinocytes and cause epithelial lesions of varying severity. Infection with a subset of high-risk mucosal alpha HPV types (e.g. HPV16 or HPV18) is the major risk factor for the development of cervical cancer (zur Hausen, 2002). Cutaneous HPVs display a much greater heterogeneity and belong to different genera. The first time that HPV infection was linked with the development of skin cancer was in the rare genetic disease epidermodysplasia verruciformis (EV). EV patients are highly susceptible to HPV infection and develop cutaneous squamous cell carcinomas (SCC), mainly on sun-exposed skin. In contrast to the diversity of bPV genotypes found in benign skin lesions, only a subset of bPVs, most frequently HPV5 (species b1) and occasionally HPV8, 14, 17, 19, 20, 24 or 47, are associated with malignant conversion to SCC in EV patients (Dell'Oste et al., 2009;Orth, 2006). UV radiation is recognized as the main risk factor in SCC development, whereas the role of HPV is less clear (Akgül et al., 2006;Pfister, 2003). Actinic keratosis is regarded as an early precancerous intraepidermal neoplasia, which represents the cutaneous counterpart of squamous intraepithelial lesions in the genital mucosa. Interestingly, the high prevalence and viral load of bPV types in these precancerous skin lesions Weissenborn et al., 2005) and the decrease in viral load during skin carcinogenesis may point to a particular involvement of HPV in the early stages of skin cancer development.Recent publications have demonstrated that bHPV-expressing keratinocytes can potentially facilitate UV radiationinduced DNA damage, as they are able to inhibit apoptosis in response to UV damage (Jackson & Storey, 2000;Leverrier et al., 2007;Struijk et al., 2008;Underbrink et al., 2008) and compromise the repair of UV-induced DNA mutations (Giampieri & Storey, 2004). These mechanisms may lead to the persistence of UV-damaged keratinocytes. Microarray analysis of the time course of keratinocytespecific gene expression after UVB irradiation revealed interleukin-8 (IL-8) family members as the most prominently induced genes coding for secreted proteins (Li et al., 2001). IL-8 is a...

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Role of HPV E6 proteins in preventing UVB-induced release of pro-apoptotic factors from the mitochondria

Cited by 73 publications

References 46 publications

Identification of the regions of the HPV 5 E6 protein involved in Bak degradation and inhibition of apoptosis

Identification of the regions of the HPV 5 E6 protein involved in Bak degradation and inhibition of apoptosis

Specific betapapillomaviruses associated with squamous cell carcinoma of the skin inhibit UVB-induced apoptosis of primary human keratinocytes

Human papillomavirus 5 and 8 E6 downregulate interleukin-8 secretion in primary human keratinocytes

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