Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function

During the human papillomavirus 16 (HPV16) life cycle, the E2 protein binds simultaneously to the viral genome and host chromatin throughout mitosis, ensuring viral genomes reside in daughter cell nuclei following cell division. Previously, we demonstrated that CK2 phosphorylation of E2 on serine 23...

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Autores principales: Prabhakar, Apurva T., James, Claire D., Fontan, Christian T., Otoa, Raymonde, Wang, Xu, Bristol, Molly L., Yeager, Calvin, Hill, Ronald D., Dubey, Aanchal, Wu, Shwu-Yuan, Chiang, Cheng-Ming, Morgan, Iain M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Virus-Cell Interactions
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10617519/
https://www.ncbi.nlm.nih.gov/pubmed/37712702
http://dx.doi.org/10.1128/jvi.00782-23
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author Prabhakar, Apurva T.
James, Claire D.
Fontan, Christian T.
Otoa, Raymonde
Wang, Xu
Bristol, Molly L.
Yeager, Calvin
Hill, Ronald D.
Dubey, Aanchal
Wu, Shwu-Yuan
Chiang, Cheng-Ming
Morgan, Iain M.
author_facet Prabhakar, Apurva T.
James, Claire D.
Fontan, Christian T.
Otoa, Raymonde
Wang, Xu
Bristol, Molly L.
Yeager, Calvin
Hill, Ronald D.
Dubey, Aanchal
Wu, Shwu-Yuan
Chiang, Cheng-Ming
Morgan, Iain M.
author_sort Prabhakar, Apurva T.
collection PubMed
description During the human papillomavirus 16 (HPV16) life cycle, the E2 protein binds simultaneously to the viral genome and host chromatin throughout mitosis, ensuring viral genomes reside in daughter cell nuclei following cell division. Previously, we demonstrated that CK2 phosphorylation of E2 on serine 23 promotes interaction with TopBP1, and that this interaction is required for optimum E2 mitotic chromatin association and plasmid segregation function. Others have implicated BRD4 in mediating the plasmid segregation function of E2 and we have demonstrated that there is a TopBP1-BRD4 complex in the cell. We therefore further investigated the role of the E2-BRD4 interaction in mediating E2 association with mitotic chromatin and plasmid segregation function. Using a combination of immunofluorescence and our novel plasmid segregation assay in U2OS and N/Tert-1 cells stably expressing a variety of E2 mutants, we report that direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for E2 association with mitotic chromatin and plasmid segregation. We also identify a novel TopBP1-mediated interaction between E2 and the BRD4 extra-terminal domain in vivo. In addition, we demonstrate for the first time that E2 plasmid segregation function occurs in human foreskin keratinocytes immortalized by HPV16. Overall, the results demonstrate that direct interaction with TopBP1 and the BRD4 CTM is required for E2 mitotic chromatin association and plasmid segregation function. Disruption of this complex offers therapeutic options for targeting segregation of viral genomes into daughter cells, potentially combating HPV16 infections and cancers that retain episomal genomes. IMPORTANCE: Human papillomavirus 16 (HPV16) is a causative agent in around 3%–4% of all human cancers, and currently, there are no anti-viral therapeutics available for combating this disease burden. In order to identify new therapeutic targets, we must increase our understanding of the HPV16 life cycle. Previously, we demonstrated that an interaction between E2 and the cellular protein TopBP1 mediates the plasmid segregation function of E2, allowing distribution of viral genomes into daughter nuclei following cell division. Here, we demonstrate that E2 interaction with an additional host protein, BRD4, is also essential for E2 segregation function, and that BRD4 exists in a complex with TopBP1. Overall, these results enhance our understanding of a critical part of the HPV16 life cycle and presents several therapeutic targets for disruption of the viral life cycle.
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spelling pubmed-106175192023-11-01 Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function Prabhakar, Apurva T. James, Claire D. Fontan, Christian T. Otoa, Raymonde Wang, Xu Bristol, Molly L. Yeager, Calvin Hill, Ronald D. Dubey, Aanchal Wu, Shwu-Yuan Chiang, Cheng-Ming Morgan, Iain M. J Virol Virus-Cell Interactions During the human papillomavirus 16 (HPV16) life cycle, the E2 protein binds simultaneously to the viral genome and host chromatin throughout mitosis, ensuring viral genomes reside in daughter cell nuclei following cell division. Previously, we demonstrated that CK2 phosphorylation of E2 on serine 23 promotes interaction with TopBP1, and that this interaction is required for optimum E2 mitotic chromatin association and plasmid segregation function. Others have implicated BRD4 in mediating the plasmid segregation function of E2 and we have demonstrated that there is a TopBP1-BRD4 complex in the cell. We therefore further investigated the role of the E2-BRD4 interaction in mediating E2 association with mitotic chromatin and plasmid segregation function. Using a combination of immunofluorescence and our novel plasmid segregation assay in U2OS and N/Tert-1 cells stably expressing a variety of E2 mutants, we report that direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for E2 association with mitotic chromatin and plasmid segregation. We also identify a novel TopBP1-mediated interaction between E2 and the BRD4 extra-terminal domain in vivo. In addition, we demonstrate for the first time that E2 plasmid segregation function occurs in human foreskin keratinocytes immortalized by HPV16. Overall, the results demonstrate that direct interaction with TopBP1 and the BRD4 CTM is required for E2 mitotic chromatin association and plasmid segregation function. Disruption of this complex offers therapeutic options for targeting segregation of viral genomes into daughter cells, potentially combating HPV16 infections and cancers that retain episomal genomes. IMPORTANCE: Human papillomavirus 16 (HPV16) is a causative agent in around 3%–4% of all human cancers, and currently, there are no anti-viral therapeutics available for combating this disease burden. In order to identify new therapeutic targets, we must increase our understanding of the HPV16 life cycle. Previously, we demonstrated that an interaction between E2 and the cellular protein TopBP1 mediates the plasmid segregation function of E2, allowing distribution of viral genomes into daughter nuclei following cell division. Here, we demonstrate that E2 interaction with an additional host protein, BRD4, is also essential for E2 segregation function, and that BRD4 exists in a complex with TopBP1. Overall, these results enhance our understanding of a critical part of the HPV16 life cycle and presents several therapeutic targets for disruption of the viral life cycle. American Society for Microbiology 2023-09-15 /pmc/articles/PMC10617519/ /pubmed/37712702 http://dx.doi.org/10.1128/jvi.00782-23 Text en Copyright © 2023 Prabhakar et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Virus-Cell Interactions
Prabhakar, Apurva T.
James, Claire D.
Fontan, Christian T.
Otoa, Raymonde
Wang, Xu
Bristol, Molly L.
Yeager, Calvin
Hill, Ronald D.
Dubey, Aanchal
Wu, Shwu-Yuan
Chiang, Cheng-Ming
Morgan, Iain M.
Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function
title Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function
title_full Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function
title_fullStr Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function
title_full_unstemmed Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function
title_short Direct interaction with the BRD4 carboxyl-terminal motif (CTM) and TopBP1 is required for human papillomavirus 16 E2 association with mitotic chromatin and plasmid segregation function
title_sort direct interaction with the brd4 carboxyl-terminal motif (ctm) and topbp1 is required for human papillomavirus 16 e2 association with mitotic chromatin and plasmid segregation function
topic Virus-Cell Interactions
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10617519/
https://www.ncbi.nlm.nih.gov/pubmed/37712702
http://dx.doi.org/10.1128/jvi.00782-23
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