Identification of a structural motif crucial for infectivity of hepatitis B viruses

Stoeckl, L.; Funk, Anneke; Kopitzki, Ariane; Brandenburg, Boerries; Oess, Stefanie; Will, Hans; Sirma, Hüseyin; Hildt, Eberhard

doi:10.1073/pnas.0509765103

Cited by 56 publications

(42 citation statements)

References 29 publications

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“…In these experiments capsids were transported by microtubule dependent motors to the nuclear membrane where they bound to NPCs, and they released their genome into the nucleus. These results were similar to studies with duck hepatitis virus (dHBV) (55,202,203). dHBV core proteins have an internal NLS as the carboxy-terminus of the HBV core (204).…”

Section: Nuclear Import Of Hepadnavirusessupporting

confidence: 87%

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

Greber

Püntener

2009

Seminars in Cell & Developmental Biology

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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.

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Section: Nuclear Import Of Hepadnavirusessupporting

confidence: 87%

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

Greber

Püntener

2009

Seminars in Cell & Developmental Biology

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“…In the absence of ideal cell and/or animal models for studying HBV infection, data concerning the early, postattachment steps in hepadnaviral entry are largely based on studies performed with DHBV in primary duck liver hepatocytes [28] . In the infection system developed by this research group, PHH can be infected naturally by HBV, and the HBV-based vector with reporter gene GFP can also easily enter the cell.…”

Section: Discussionmentioning

confidence: 99%

High expression of hepatitis B virus based vector with reporter gene in hepatitis B virus infection system

Huang²,

Han³

et al. 2007

WJG

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AIM:To construct a hepatitis B virus (HBV)-based vector with a reporter gene and to establish an HBV infection system to evaluate the availability of the vector. METHODS:T h e H B V-b a s e d ve c t o r s w i t h g r e e n fluorescence protein (GFP) were packaged into the liver of immunodeficient mice through transfer and helper plasmid using hydrodynamic technology. Wild type HBV (wt HBV) was provided by plasmid MC2009. Primary human hepatocytes (PHH) were isolated and infected with recombinant HBV (rHBV) or wt HBV. GFP expression was monitored by confocal and flow cytometry. HBV DNA and HBV surface antigen (HBSAg) were analyzed by PCR and ELISA. RESULTS: 3 × 107 wt HBV copies/mL and 5 × 10 6 rHBV copies/mL were collected from mice serum. In the wt HBV infected group, HBV progeny was 2 × 10 7 copies/mL and HBSAg was 770 ng/mL. In the rHBV infected group, GFP fluorescence was detected on d 3 post-infection and over 85% of the parenchymal cells expressed green fluorescence on d 12 post-infection. Compared with wt HBV in the PHH infection system, no rHBV DNA or HBSAg were detected in PHH culture media.CONCLUSION: An effective HBV based vector was developed, which proved to be a useful HBV infection system. This vector and infection system can be applied to develop a therapeutic vector and study the HBV life cycle and viral pathogenesis.

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“…So far, this cellular receptor as not been identified. Proteolytic cleavage of the surface protein occurs within the endosomal compartment, probably resulting in a conformational change that exposes some translocation motifs at the surface of the viral particle allowing fusion of viral and cellular membranes and release of the capsid into the cytosol (Stoeckl et al, 2006). The naked capsid is then directed towards the nucleus, and the HBV genome is translocated to the nucleus (Rabe et al, 2006).…”

Section: Overview Of the Hepatitis B Virus Life Cyclementioning

confidence: 99%

Hepatitis B Virus X Protein: A Key Regulator of the Virus Life Cycle

Protzer¹

2012

Viral Genomes - Molecular Structure, Diversity, Gene Expression Mechanisms and Host-Virus Interactions

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Identification of a structural motif crucial for infectivity of hepatitis B viruses

Cited by 56 publications

References 29 publications

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

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

High expression of hepatitis B virus based vector with reporter gene in hepatitis B virus infection system

Hepatitis B Virus X Protein: A Key Regulator of the Virus Life Cycle

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