Expression, Enzymatic Activities and Subcellular Localization of Hepatitis E Virus and Semliki Forest Virus Replicase Proteins
| Contribuinte(s) |
Helsingin yliopisto, biotieteellinen tiedekunta, bio- ja ympäristötieteiden laitos University of Helsinki, Faculty of Biosciences, Department of Biological and Environmental Sciences, General Microbiology Helsingfors universitet, biovetenskapliga fakulteten, institutionen för bio- och miljövetenskaper |
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| Data(s) |
23/02/2006
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| Resumo |
Viruses are submicroscopic, infectious agents that are obligate intracellular parasites. They adopt various types of strategies for their parasitic replication and proliferation in infected cells. The nucleic acid genome of a virus contains information that redirects molecular machinery of the cell to the replication and production of new virions. Viruses that replicate in the cytoplasm and are unable to use the nuclear transcription machinery of the host cell have developed their own transcription and capping systems. This thesis describes replication strategies of two distantly related viruses, hepatitis E virus (HEV) and Semliki Forest virus (SFV), which belong to the alphavirus-like superfamily of positive-strand RNA viruses. We have demonstrated that HEV and SFV share a unique cap formation pathway specific for alphavirus-like superfamily. The capping enzyme first acts as a methyltransferase, catalyzing the transfer of a methyl group from S-adenosylmethionine to GTP to yield m7GTP. It then transfers the methylated guanosine to the end of viral mRNA. Both reactions are virus-specific and differ from those described for the host cell. Therefore, these capping reactions offer attractive targets for the development of antiviral drugs. Additionally, it has been shown that replication of SFV and HEV takes place in association with cellular membranes. The origin of these membranes and the intracellular localization of the components of the replication complex were studied by modern microscopy techniques. It was demonstrated that SFV replicates in cytoplasmic membranes that are derived from endosomes and lysosomes. According to our studies, site for HEV replication seems to be the intermediate compartment which mediates the traffic between endoplasmic reticulum and the Golgi complex. As a result of this work, a unique mechanism of cap formation for hepatitis E virus replicase has been characterized. It represents a novel target for the development of specific inhibitors against viral replication. |
| Identificador |
URN:ISBN:952-10-2941-2 |
| Idioma(s) |
en |
| Publicador |
Helsingin yliopisto University of Helsinki Helsingfors universitet |
| Relação |
Gummerus Printing: Julia Perttilä, 2006, Dissertationes bioscientiarum molecularium Universitatis Helsingiensis in Viikki URN:ISBN:952-10-2940-4 |
| Direitos |
Julkaisu on tekijänoikeussäännösten alainen. Teosta voi lukea ja tulostaa henkilökohtaista käyttöä varten. Käyttö kaupallisiin tarkoituksiin on kielletty. This publication is copyrighted. You may download, display and print it for Your own personal use. Commercial use is prohibited. Publikationen är skyddad av upphovsrätten. Den får läsas och skrivas ut för personligt bruk. Användning i kommersiellt syfte är förbjuden. |
| Palavras-Chave | #Yleinen mikrobiologia |
| Tipo |
Väitöskirja (artikkeli) Doctoral dissertation (article-based) Doktorsavhandling (sammanläggning) Text |
