The Human Papillomavirus Type 8 E6 Protein Interferes with NOTCH Activation during Keratinocyte Differentiation

Meyers, Jordan M.; Spangle, Jennifer M.; Münger, Karl

doi:10.1128/jvi.02527-12

Cited by 84 publications

(73 citation statements)

References 20 publications

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“…These novel findings indicate consistent activation of the Notch signaling pathway, with increases in downstream targets driven by increased NFX1-123 that was reduced in parallel when NFX1-123 and Notch1 were decreased. Interestingly, the Notch1 transcription protein partner MAML is bound and targeted for degradation by beta-HPV E6 types to inhibit Notch signaling (50)(51)(52)(53); however, alpha-HPV E6 scramble short hairpin RNA control (scr), sh1RNA to NFX1-123 (sh1), or sh2RNA to NFX1-123 (sh2). Relative levels of Hes1 mRNA were calculated using the ⌬⌬C T method, normalizing mRNA levels to GAPDH within each sample.…”

Section: Discussionmentioning

confidence: 99%

NFX1-123 and Human Papillomavirus 16E6 Increase Notch Expression in Keratinocytes

Vliet-Gregg¹,

Hamilton²,

Katzenellenbogen

2013

J Virol

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The high-risk human papillomavirus (HR HPV) E6 oncoprotein binds host cell proteins to dysregulate multiple regulatory pathways, including apoptosis and senescence. HR HPV16 E6 (16E6) interacts with the cellular protein NFX1-123, and together they posttranscriptionally increase hTERT expression, the catalytic subunit of telomerase. NFX1-123 interacts with hTERT mRNA and stabilizes it, leading to greater telomerase activity and the avoidance of cellular senescence. Little is known regarding what other transcripts are dependent on or augmented by the association of NFX1-123 with 16E6. Microarray analysis revealed enhanced expression of Notch1 mRNA in 16E6-expressing keratinocytes when NFX1-123 was overexpressed. A moderate increase in Notch1 mRNA was seen with overexpression of NFX1-123 alone, but with 16E6 coexpression the increase in Notch1 was enhanced. The PAM2 motif and R3H protein domains in NFX1-123, which were important for increased hTERT expression, were also important in the augmentation of Notch1 expression by 16E6. These findings identify a second gene coregulated by 16E6 and NFX1-123 and the protein motifs in NFX1-123 that are important for this effect. Human papillomaviruses (HPVs) are nonenveloped doublestranded DNA viruses. Of the more than 150 HPVs that have been identified to date, over 30 types are capable of infecting the genital and oral mucosa. HPVs that infect mucosa are divided into low-risk (LR) and high-risk (HR) categories based on their associated risk for anogenital and, increasingly, head and neck cancers (1-11). As these HR HPV infections are linked to malignancies, much focus has been placed on studying the cellular changes these viruses trigger that lead to cancer and on studying the functions of two oncogenes expressed by HR HPV, E6 and E7.HR E6 induces oncogenic changes primarily through its interactions with host cell proteins, and those interactions block apoptotic signaling and drive cellular immortalization (for a review, see reference 12). E6-associated protein (E6AP) is an E3 ubiquitin ligase that is the most well-studied protein partner of HR E6 (13-19). However, HR E6 interacts with other cellular proteins, such as NFX1 splice variants, and these are important in oncogenesis as well (20,21).In human epithelial cells, NFX1 is a gene expressed as two splice variants, . NFX1-91 has been shown to transcriptionally repress telomerase expression in epithelial cells, and HR HPV 16E6 with E6AP targets NFX1-91 for degradation (22,23). Our work has focused on NFX1-123, the longer splice variant of NFX1, and on its role with 16E6 in oncogenesis. Previously we had shown that 16E6 bound NFX1-123 in its central domain, but unlike NFX1-91 it was not degraded; together, 16E6 and NFX1-123 increased hTERT expression and telomerase activity in human foreskin keratinocytes (HFKs) through a posttranscriptional mechanism (20). 16E6 and NFX1-123 increased hTERT by utilizing both the PAM2 motif and R3H domain of the NFX1-123 protein. The N-terminal PAM2 motif is required to interact with cytopl...

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Section: Discussionmentioning

confidence: 99%

NFX1-123 and Human Papillomavirus 16E6 Increase Notch Expression in Keratinocytes

Vliet-Gregg¹,

Hamilton²,

Katzenellenbogen

2013

J Virol

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“…In addition, some beta-HPV E6 proteins have also been reported to cause degradation of the transcriptional coactivator p300, thereby short-circuiting DNA repair in response to UV damage by the Ataxia telangiectasia and Rad3-related kinase (Wallace et al, 2012;Howie et al, 2011). More recently, some beta-HPV E6 proteins have also been shown to inhibit NOTCH signaling, which is important for epithelial cell differentiation and stem cell maintenance (Meyers et al, 2013;Tan et al, 2012;Brimer et al, 2012).…”

Section: Beta-hpvs and Skin Cancersmentioning

confidence: 96%

Papillomaviruses

McLaughlin-Drubin¹,

Munger²

2014

Reference Module in Biomedical Sciences

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“…One of the critical regulators of epithelial differentiation is NOTCH signaling. Several recent studies have shown that the HPV5 and HPV8 E6 proteins inhibit NOTCH signaling by interacting with MAML proteins, critical co-activators of the NOTCH transcription complex (Brimer et al, 2012;Rozenblatt-Rosen et al, 2012;Tan et al, 2012;Meyers et al, 2013). NOTCH has tumor suppressor activities in epithelia, and inactivating NOTCH pathway mutations are highly prevalent in SCCs (Agrawal et al, 2011;Stransky et al, 2011).…”

Section: Beta Human Papillomaviruses and Non-melanoma Skin Cancersmentioning

confidence: 99%

The Viral Etiology of Skin Cancer

Meyers

Münger

2014

Journal of Investigative Dermatology

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The Human Papillomavirus Type 8 E6 Protein Interferes with NOTCH Activation during Keratinocyte Differentiation

Cited by 84 publications

References 20 publications

NFX1-123 and Human Papillomavirus 16E6 Increase Notch Expression in Keratinocytes

NFX1-123 and Human Papillomavirus 16E6 Increase Notch Expression in Keratinocytes

Papillomaviruses

The Viral Etiology of Skin Cancer

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