Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.

Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.

Zaire ebolavirus (ZEBOV) infections are associated with high lethality in primates. ZEBOV primarily targets mononuclear phagocytes, which are activated upon infection and secrete mediators believed to trigger initial stages of pathogenesis. The characterization of the responses of target cells to ZE...

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Main Authors: Victoria Wahl-Jensen, Sabine Kurz, Friedericke Feldmann, Lukas K Buehler, Jason Kindrachuk, Victor DeFilippis, Jean da Silva Correia, Klaus Früh, Jens H Kuhn, Dennis R Burton, Heinz Feldmann
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-10-01
Series:PLoS Neglected Tropical Diseases
Online Access:http://europepmc.org/articles/PMC3196478?pdf=render
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spelling doaj-8af603476fbf4758bad061ab860e98952020-11-25T00:07:28ZengPublic Library of Science (PLoS)PLoS Neglected Tropical Diseases1935-27271935-27352011-10-01510e135910.1371/journal.pntd.0001359Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.Victoria Wahl-JensenSabine KurzFriedericke FeldmannLukas K BuehlerJason KindrachukVictor DeFilippisJean da Silva CorreiaKlaus FrühJens H KuhnDennis R BurtonHeinz FeldmannZaire ebolavirus (ZEBOV) infections are associated with high lethality in primates. ZEBOV primarily targets mononuclear phagocytes, which are activated upon infection and secrete mediators believed to trigger initial stages of pathogenesis. The characterization of the responses of target cells to ZEBOV infection may therefore not only further understanding of pathogenesis but also suggest possible points of therapeutic intervention. Gene expression profiles of primary human macrophages exposed to ZEBOV were determined using DNA microarrays and quantitative PCR to gain insight into the cellular response immediately after cell entry. Significant changes in mRNA concentrations encoding for 88 cellular proteins were observed. Most of these proteins have not yet been implicated in ZEBOV infection. Some, however, are inflammatory mediators known to be elevated during the acute phase of disease in the blood of ZEBOV-infected humans. Interestingly, the cellular response occurred within the first hour of Ebola virion exposure, i.e. prior to virus gene expression. This observation supports the hypothesis that virion binding or entry mediated by the spike glycoprotein (GP(1,2)) is the primary stimulus for an initial response. Indeed, ZEBOV virions, LPS, and virus-like particles consisting of only the ZEBOV matrix protein VP40 and GP(1,2) (VLP(VP40-GP)) triggered comparable responses in macrophages, including pro-inflammatory and pro-apoptotic signals. In contrast, VLP(VP40) (particles lacking GP(1,2)) caused an aberrant response. This suggests that GP(1,2) binding to macrophages plays an important role in the immediate cellular response.http://europepmc.org/articles/PMC3196478?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Victoria Wahl-Jensen
Sabine Kurz
Friedericke Feldmann
Lukas K Buehler
Jason Kindrachuk
Victor DeFilippis
Jean da Silva Correia
Klaus Früh
Jens H Kuhn
Dennis R Burton
Heinz Feldmann
spellingShingle Victoria Wahl-Jensen
Sabine Kurz
Friedericke Feldmann
Lukas K Buehler
Jason Kindrachuk
Victor DeFilippis
Jean da Silva Correia
Klaus Früh
Jens H Kuhn
Dennis R Burton
Heinz Feldmann
Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.
PLoS Neglected Tropical Diseases
author_facet Victoria Wahl-Jensen
Sabine Kurz
Friedericke Feldmann
Lukas K Buehler
Jason Kindrachuk
Victor DeFilippis
Jean da Silva Correia
Klaus Früh
Jens H Kuhn
Dennis R Burton
Heinz Feldmann
author_sort Victoria Wahl-Jensen
title Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.
title_short Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.
title_full Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.
title_fullStr Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.
title_full_unstemmed Ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.
title_sort ebola virion attachment and entry into human macrophages profoundly effects early cellular gene expression.
publisher Public Library of Science (PLoS)
series PLoS Neglected Tropical Diseases
issn 1935-2727
1935-2735
publishDate 2011-10-01
description Zaire ebolavirus (ZEBOV) infections are associated with high lethality in primates. ZEBOV primarily targets mononuclear phagocytes, which are activated upon infection and secrete mediators believed to trigger initial stages of pathogenesis. The characterization of the responses of target cells to ZEBOV infection may therefore not only further understanding of pathogenesis but also suggest possible points of therapeutic intervention. Gene expression profiles of primary human macrophages exposed to ZEBOV were determined using DNA microarrays and quantitative PCR to gain insight into the cellular response immediately after cell entry. Significant changes in mRNA concentrations encoding for 88 cellular proteins were observed. Most of these proteins have not yet been implicated in ZEBOV infection. Some, however, are inflammatory mediators known to be elevated during the acute phase of disease in the blood of ZEBOV-infected humans. Interestingly, the cellular response occurred within the first hour of Ebola virion exposure, i.e. prior to virus gene expression. This observation supports the hypothesis that virion binding or entry mediated by the spike glycoprotein (GP(1,2)) is the primary stimulus for an initial response. Indeed, ZEBOV virions, LPS, and virus-like particles consisting of only the ZEBOV matrix protein VP40 and GP(1,2) (VLP(VP40-GP)) triggered comparable responses in macrophages, including pro-inflammatory and pro-apoptotic signals. In contrast, VLP(VP40) (particles lacking GP(1,2)) caused an aberrant response. This suggests that GP(1,2) binding to macrophages plays an important role in the immediate cellular response.
url http://europepmc.org/articles/PMC3196478?pdf=render
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