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Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor

It has been proposed that some non-retroviral RNA virus genes are integrated into vertebrate genomes. Endogenous filovirus-like elements (EFLs) have been discovered in some mammalian genomes. However, their potential roles in ebolavirus infection are unclear. A filovirus VP35-like element (mlEFL35)...

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Autores principales: Kondoh, Tatsunari, Manzoor, Rashid, Nao, Naganori, Maruyama, Junki, Furuyama, Wakako, Miyamoto, Hiroko, Shigeno, Asako, Kuroda, Makoto, Matsuno, Keita, Fujikura, Daisuke, Kajihara, Masahiro, Yoshida, Reiko, Igarashi, Manabu, Takada, Ayato
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5645129/
https://www.ncbi.nlm.nih.gov/pubmed/29040311
http://dx.doi.org/10.1371/journal.pone.0186450
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author Kondoh, Tatsunari
Manzoor, Rashid
Nao, Naganori
Maruyama, Junki
Furuyama, Wakako
Miyamoto, Hiroko
Shigeno, Asako
Kuroda, Makoto
Matsuno, Keita
Fujikura, Daisuke
Kajihara, Masahiro
Yoshida, Reiko
Igarashi, Manabu
Takada, Ayato
author_facet Kondoh, Tatsunari
Manzoor, Rashid
Nao, Naganori
Maruyama, Junki
Furuyama, Wakako
Miyamoto, Hiroko
Shigeno, Asako
Kuroda, Makoto
Matsuno, Keita
Fujikura, Daisuke
Kajihara, Masahiro
Yoshida, Reiko
Igarashi, Manabu
Takada, Ayato
author_sort Kondoh, Tatsunari
collection PubMed
description It has been proposed that some non-retroviral RNA virus genes are integrated into vertebrate genomes. Endogenous filovirus-like elements (EFLs) have been discovered in some mammalian genomes. However, their potential roles in ebolavirus infection are unclear. A filovirus VP35-like element (mlEFL35) is found in the little brown bat (Myotis lucifugus) genome. Putative mlEFL35-derived protein (mlEFL35p) contains nearly full-length amino acid sequences corresponding to ebolavirus VP35. Ebola virus VP35 has been shown to bind double-stranded RNA, leading to inhibition of type I interferon (IFN) production, and is also known as a viral polymerase cofactor that is essential for viral RNA transcription/replication. In this study, we transiently expressed mlEFL35p in human kidney cells and investigated its biological functions. We first found that mlEFL35p was coimmunoprecipitated with itself and ebolavirus VP35s but not with the viral nucleoprotein. Then the biological functions of mlEFL35p were analyzed by comparing it to ebolavirus VP35s. We found that the expression of mlEFL35p significantly inhibited human IFN-β promoter activity as well as VP35s. By contrast, expression of mlEFL35p did not support viral RNA transcription/replication and indeed slightly decrease the reporter gene expression in a minigenome assay. These results suggest that mlEFL35p potentially acts as an IFN antagonist but not a polymerase cofactor.
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spelling pubmed-56451292017-10-30 Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor Kondoh, Tatsunari Manzoor, Rashid Nao, Naganori Maruyama, Junki Furuyama, Wakako Miyamoto, Hiroko Shigeno, Asako Kuroda, Makoto Matsuno, Keita Fujikura, Daisuke Kajihara, Masahiro Yoshida, Reiko Igarashi, Manabu Takada, Ayato PLoS One Research Article It has been proposed that some non-retroviral RNA virus genes are integrated into vertebrate genomes. Endogenous filovirus-like elements (EFLs) have been discovered in some mammalian genomes. However, their potential roles in ebolavirus infection are unclear. A filovirus VP35-like element (mlEFL35) is found in the little brown bat (Myotis lucifugus) genome. Putative mlEFL35-derived protein (mlEFL35p) contains nearly full-length amino acid sequences corresponding to ebolavirus VP35. Ebola virus VP35 has been shown to bind double-stranded RNA, leading to inhibition of type I interferon (IFN) production, and is also known as a viral polymerase cofactor that is essential for viral RNA transcription/replication. In this study, we transiently expressed mlEFL35p in human kidney cells and investigated its biological functions. We first found that mlEFL35p was coimmunoprecipitated with itself and ebolavirus VP35s but not with the viral nucleoprotein. Then the biological functions of mlEFL35p were analyzed by comparing it to ebolavirus VP35s. We found that the expression of mlEFL35p significantly inhibited human IFN-β promoter activity as well as VP35s. By contrast, expression of mlEFL35p did not support viral RNA transcription/replication and indeed slightly decrease the reporter gene expression in a minigenome assay. These results suggest that mlEFL35p potentially acts as an IFN antagonist but not a polymerase cofactor. Public Library of Science 2017-10-17 /pmc/articles/PMC5645129/ /pubmed/29040311 http://dx.doi.org/10.1371/journal.pone.0186450 Text en © 2017 Kondoh et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Kondoh, Tatsunari
Manzoor, Rashid
Nao, Naganori
Maruyama, Junki
Furuyama, Wakako
Miyamoto, Hiroko
Shigeno, Asako
Kuroda, Makoto
Matsuno, Keita
Fujikura, Daisuke
Kajihara, Masahiro
Yoshida, Reiko
Igarashi, Manabu
Takada, Ayato
Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor
title Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor
title_full Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor
title_fullStr Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor
title_full_unstemmed Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor
title_short Putative endogenous filovirus VP35-like protein potentially functions as an IFN antagonist but not a polymerase cofactor
title_sort putative endogenous filovirus vp35-like protein potentially functions as an ifn antagonist but not a polymerase cofactor
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5645129/
https://www.ncbi.nlm.nih.gov/pubmed/29040311
http://dx.doi.org/10.1371/journal.pone.0186450
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