DNA-tumor virus entry—From plasma membrane to the nucleus

DNA-tumor viruses comprise enveloped and non-enveloped agents that cause malignancies in a large variety of cell types and tissues by interfering with cell cycle control and immortalization. Those DNA-tumor viruses that replicate in the nucleus use cellular mechanisms to transport their genome and n...

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Bibliographic Details
Published in:Seminars in cell & developmental biology 2009-07, Vol.20 (5), p.631-642
Main Authors: Puntener, Daniel, Greber, Urs F.
Format: Article
Language:English
Subjects:
Active Transport, Cell Nucleus
Cell Membrane - metabolism
Cell Membrane - virology
Cell Nucleus - metabolism
Cell Nucleus - virology
Cell transformation
Cytoplasmic transport
DNA Tumor Viruses - metabolism
Nuclear Pore - metabolism
Nuclear Pore - virology
Nuclear pore complex
Nucleocytoplasmic transport
Virus entry
Virus Internalization
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Summary:DNA-tumor viruses comprise enveloped and non-enveloped agents that cause malignancies in a large variety of cell types and tissues by interfering with cell cycle control and immortalization. Those DNA-tumor viruses that replicate in the nucleus use cellular mechanisms to transport their genome and newly synthesized viral proteins into the nucleus. This requires cytoplasmic transport and nuclear import of their genome. Agents that employ this strategy include adenoviruses, hepadnaviruses, herpesviruses, and likely also papillomaviruses, and polyomaviruses, but not poxviruses which replicate in the cytoplasm. Here, we discuss how DNA-tumor viruses enter cells, take advantage of cytoplasmic transport, and import their DNA genome through the nuclear pore complex into the nucleus. Remarkably, nuclear import of incoming genomes does not necessarily follow the same pathways used by the structural proteins of the viruses during the replication and assembly phases of the viral life cycle. Understanding the mechanisms of DNA nuclear import can identify new pathways of cell regulation and anti-viral therapies.
ISSN:1084-9521
1096-3634
DOI:10.1016/j.semcdb.2009.03.014