Inhibition zellulärer antiviraler Abwehrmechanismen durch das Hepatitis A-Virus - eine Analyse der beteiligten viralen Faktoren: Inhibition des IRF-3 -vermittelten Signalweges durch das Nichtstrukturprotein 2B des Hepatitis A-Virus
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Sonstige Titel: | Analysis of the inhibition of cellular antiviral mechanisms by the Hepatitis A-Virus: Inhibition of the IRF-3-mediated signalling pathway by the nonstructural protein 2B of HAV | Autor/Autorin: | Magulski, Thomas | BetreuerIn: | Vallbracht, Angelika | 1. GutachterIn: | Vallbracht, Angelika | Weitere Gutachter:innen: | Schmitz, Herbert | Zusammenfassung: | Hepatitis A virus (HAV) antagonizes the innate immune response by inhibition of Newcastle disease virus (NDV)- or dsRNA-mediated interferon-beta (IFN-beta) gene expression. The aim of this dissertation was to investigate which viral properties or factors are involved in this suppression. It could be demonstrated that the nonstructural protein HAV-2B correlates with the ability of HAV to suppress the NDV- or dsRNA-mediated interferon-beta (IFN-beta) gene expression. Further investigations supported this finding that HAV-2B is involved in inhibition of activation of transcription factor IRF-3 by HAV. As IRF-3 is necessary for IFN-beta transcription, inhibition of this factor results in efficient suppression of IFN-beta synthesis. This ability might be of vital importance for HAV, which is an exceptionally slowly growing virus sensitive to IFN-beta, as it allows this virus to establish infection and maintain viral replication for a longer time. |
Schlagwort: | HAV; Hepatitis A-Virus; IRF-3; HAV-2B; Interferon; dsRNA; RIG-I; innate immune response | Veröffentlichungsdatum: | 19-Dez-2007 | Dokumenttyp: | Dissertation | Zweitveröffentlichung: | no | URN: | urn:nbn:de:gbv:46-diss000108829 | Institution: | Universität Bremen | Fachbereich: | Fachbereich 02: Biologie/Chemie (FB 02) |
Enthalten in den Sammlungen: | Dissertationen |
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