CREB1 activation promotes human papillomavirus oncogene expression and cervical cancer cell transformation

Human papillomaviruses (HPVs) infect the oral and anogenital mucosa and can cause cancer. The high‐risk (HR)‐HPV oncoproteins, E6 and E7, hijack cellular factors to promote cell proliferation, delay differentiation and induce genomic instability, thus predisposing infected cells to malignant transfo...

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Veröffentlicht in:	Journal of medical virology 2023-08, Vol.95 (8), p.e29025-n/a
Hauptverfasser:	Li, Yigen, Patterson, Molly R., Morgan, Ethan L., Wasson, Christopher W., Ryder, Emma L., Barba‐Moreno, Diego, Scarth, James A., Wang, Miao, Macdonald, Andrew
Format:	Artikel
Sprache:	eng
Schlagworte:	Anogenital Cancer Cell differentiation Cell growth Cell proliferation Cervical cancer Control theory CREB1 Cyclic AMP response element-binding protein Cyclic AMP Response Element-Binding Protein - genetics Epithelial-Mesenchymal Transition Feedback loops Female Genomic instability Health risks HPV Human papillomavirus Human Papillomavirus Viruses Humans Keratinocytes Life cycle analysis MAP kinase miRNA miR‐203a Oncogene Proteins, Viral - genetics Oncogenes Oncoproteins Papillomaviridae Papillomavirus E7 Proteins - genetics Papillomavirus Infections Phosphorylation Positive feedback Repressor Proteins - genetics Ribonucleic acid RNA Tumor cell lines Tumor suppressor genes Uterine Cervical Neoplasms Virology
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creator	Li, Yigen Patterson, Molly R. Morgan, Ethan L. Wasson, Christopher W. Ryder, Emma L. Barba‐Moreno, Diego Scarth, James A. Wang, Miao Macdonald, Andrew
description	Human papillomaviruses (HPVs) infect the oral and anogenital mucosa and can cause cancer. The high‐risk (HR)‐HPV oncoproteins, E6 and E7, hijack cellular factors to promote cell proliferation, delay differentiation and induce genomic instability, thus predisposing infected cells to malignant transformation. cAMP response element (CRE)‐binding protein 1 (CREB1) is a master transcription factor that can function as a proto‐oncogene, the abnormal activity of which is associated with multiple cancers. However, little is known about the interplay between HPV and CREB1 activity in cervical cancer or the productive HPV lifecycle. We show that CREB is activated in productively infected primary keratinocytes and that CREB1 expression and phosphorylation is associated with the progression of HPV+ cervical disease. The depletion of CREB1 or inhibition of CREB1 activity results in decreased cell proliferation and reduced expression of markers of epithelial to mesenchymal transition, coupled with reduced migration in HPV+ cervical cancer cell lines. CREB1 expression is negatively regulated by the tumor suppressor microRNA, miR‐203a, and CREB1 phosphorylation is controlled through the MAPK/MSK pathway. Crucially, CREB1 directly binds the viral promoter to upregulate transcription of the E6/E7 oncogenes, establishing a positive feedback loop between the HPV oncoproteins and CREB1. Our findings demonstrate the oncogenic function of CREB1 in HPV+ cervical cancer and its relationship with the HPV oncogenes.
doi_str_mv	10.1002/jmv.29025
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The high‐risk (HR)‐HPV oncoproteins, E6 and E7, hijack cellular factors to promote cell proliferation, delay differentiation and induce genomic instability, thus predisposing infected cells to malignant transformation. cAMP response element (CRE)‐binding protein 1 (CREB1) is a master transcription factor that can function as a proto‐oncogene, the abnormal activity of which is associated with multiple cancers. However, little is known about the interplay between HPV and CREB1 activity in cervical cancer or the productive HPV lifecycle. We show that CREB is activated in productively infected primary keratinocytes and that CREB1 expression and phosphorylation is associated with the progression of HPV+ cervical disease. The depletion of CREB1 or inhibition of CREB1 activity results in decreased cell proliferation and reduced expression of markers of epithelial to mesenchymal transition, coupled with reduced migration in HPV+ cervical cancer cell lines. CREB1 expression is negatively regulated by the tumor suppressor microRNA, miR‐203a, and CREB1 phosphorylation is controlled through the MAPK/MSK pathway. Crucially, CREB1 directly binds the viral promoter to upregulate transcription of the E6/E7 oncogenes, establishing a positive feedback loop between the HPV oncoproteins and CREB1. Our findings demonstrate the oncogenic function of CREB1 in HPV+ cervical cancer and its relationship with the HPV oncogenes.</description><identifier>ISSN: 0146-6615</identifier><identifier>EISSN: 1096-9071</identifier><identifier>DOI: 10.1002/jmv.29025</identifier><identifier>PMID: 37565725</identifier><language>eng</language><publisher>United States: Wiley Subscription Services, Inc</publisher><subject>Anogenital ; Cancer ; Cell differentiation ; Cell growth ; Cell proliferation ; Cervical cancer ; Control theory ; CREB1 ; Cyclic AMP response element-binding protein ; Cyclic AMP Response Element-Binding Protein - genetics ; Epithelial-Mesenchymal Transition ; Feedback loops ; Female ; Genomic instability ; Health risks ; HPV ; Human papillomavirus ; Human Papillomavirus Viruses ; Humans ; Keratinocytes ; Life cycle analysis ; MAP kinase ; miRNA ; miR‐203a ; Oncogene Proteins, Viral - genetics ; Oncogenes ; Oncoproteins ; Papillomaviridae ; Papillomavirus E7 Proteins - genetics ; Papillomavirus Infections ; Phosphorylation ; Positive feedback ; Repressor Proteins - genetics ; Ribonucleic acid ; RNA ; Tumor cell lines ; Tumor suppressor genes ; Uterine Cervical Neoplasms ; Virology</subject><ispartof>Journal of medical virology, 2023-08, Vol.95 (8), p.e29025-n/a</ispartof><rights>2023 The Authors. published by Wiley Periodicals LLC.</rights><rights>2023 The Authors. 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The high‐risk (HR)‐HPV oncoproteins, E6 and E7, hijack cellular factors to promote cell proliferation, delay differentiation and induce genomic instability, thus predisposing infected cells to malignant transformation. cAMP response element (CRE)‐binding protein 1 (CREB1) is a master transcription factor that can function as a proto‐oncogene, the abnormal activity of which is associated with multiple cancers. However, little is known about the interplay between HPV and CREB1 activity in cervical cancer or the productive HPV lifecycle. We show that CREB is activated in productively infected primary keratinocytes and that CREB1 expression and phosphorylation is associated with the progression of HPV+ cervical disease. The depletion of CREB1 or inhibition of CREB1 activity results in decreased cell proliferation and reduced expression of markers of epithelial to mesenchymal transition, coupled with reduced migration in HPV+ cervical cancer cell lines. CREB1 expression is negatively regulated by the tumor suppressor microRNA, miR‐203a, and CREB1 phosphorylation is controlled through the MAPK/MSK pathway. Crucially, CREB1 directly binds the viral promoter to upregulate transcription of the E6/E7 oncogenes, establishing a positive feedback loop between the HPV oncoproteins and CREB1. 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subjects	Anogenital Cancer Cell differentiation Cell growth Cell proliferation Cervical cancer Control theory CREB1 Cyclic AMP response element-binding protein Cyclic AMP Response Element-Binding Protein - genetics Epithelial-Mesenchymal Transition Feedback loops Female Genomic instability Health risks HPV Human papillomavirus Human Papillomavirus Viruses Humans Keratinocytes Life cycle analysis MAP kinase miRNA miR‐203a Oncogene Proteins, Viral - genetics Oncogenes Oncoproteins Papillomaviridae Papillomavirus E7 Proteins - genetics Papillomavirus Infections Phosphorylation Positive feedback Repressor Proteins - genetics Ribonucleic acid RNA Tumor cell lines Tumor suppressor genes Uterine Cervical Neoplasms Virology
title	CREB1 activation promotes human papillomavirus oncogene expression and cervical cancer cell transformation
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