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Título: SOX2 as a New Regulator of HPV16 Transcription
Autor(es): MARTINEZ RAMIREZ, IMELDA
DEL CASTILLO FALCONI, VICTOR MANUEL
MITRE AGUILAR, IRMA BEATRIZ
AMADOR MOLINA, ALFREDO
CARRILLO GARCIA, ADELA LUCIA
LANGLEY MCCARRON, ELIZABETH
ZENTELLA DEHESA, ALEJANDRO
SOTO REYES SOLIS, ERNESTO
GARCIA CARRANCA, ALEJANDRO MANUEL
HERRERA MONTALVO, LUIS ALONSO
LIZANO SOBERANO, MARCELA
Temas: Virus del papiloma humano
VPH
LCR
SOX2
Regulación transcripcional
Fecha: 2017
Editorial: Basilea : MDPI
Citation: Viruses, 9(7), 2017
Resumen: Persistent infections with high-risk human papillomavirus (HPV) constitute the main risk factor for cervical cancer development. HPV16 is the most frequent type associated to squamous cell carcinomas (SCC), followed by HPV18. The long control region (LCR) in the HPV genome contains the replication origin and sequences recognized by cellular transcription factors (TFs) controlling viral transcription. Altered expression of E6 and E7 viral oncogenes, modulated by the LCR, causes modifications in cellular pathways such as proliferation, leading to malignant transformation. The aim of this study was to identify specific TFs that could contribute to the modulation of high-risk HPV transcriptional activity, related to the cellular histological origin. We identified sex determining region Y (SRY)-box 2 (SOX2) response elements present in HPV16-LCR. SOX2 binding to the LCR was demonstrated by in vivo and in vitro assays. The overexpression of this TF repressed HPV16-LCR transcriptional activity, as shown through reporter plasmid assays and by the down-regulation of endogenous HPV oncogenes. Site-directed mutagenesis revealed that three putative SOX2 binding sites are involved in the repression of the LCR activity. We propose that SOX2 acts as a transcriptional repressor of HPV16-LCR, decreasing the expression of E6 and E7 oncogenes in a SCC context.
URI: http://ilitia.cua.uam.mx:8080/jspui/handle/123456789/903
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