Literature DB >> 12050362

Turnover of hepatitis B virus X protein is regulated by damaged DNA-binding complex.

Françoise Bergametti1, Delphine Sitterlin, Catherine Transy.   

Abstract

Mammalian hepatitis B viruses encode an essential regulatory protein, termed X, which may also be implicated in liver cancer development associated with chronic infection. X protein, also referred to as HBx in human virus and WHx in woodchuck virus, has been reported to bind to a number of cellular proteins, including the DDB1 subunit of the damaged DNA-binding (DDB) complex. Our previous work provided genetic evidence for the importance of WHx-DDB1 interaction in both the activity of the X protein and establishment of viral infection in woodchucks. In the present study, a direct action of DDB1 on the X protein is documented. Physical interaction between the two proteins leads to an increase in X protein stability. This effect results from protection of the viral protein from proteasome-mediated degradation. Protection of WHx is overcome in the presence DDB2, the second subunit of the DDB heterodimer. In keeping with observations reported for HBx, DDB2 was found to directly bind to WHx. Nonetheless, the counteracting effect of DDB2 on X stabilization requires DDB2-DDB1 interaction. Taken together, these findings substantiate the physical and functional connection between the X protein and the DDB1-DDB2 heterodimer, leading to the regulation of the pool of the viral protein.

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Year:  2002        PMID: 12050362      PMCID: PMC136256          DOI: 10.1128/jvi.76.13.6495-6501.2002

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  48 in total

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5.  Hepatitis B virus X protein is both a substrate and a potential inhibitor of the proteasome complex.

Authors:  Z Hu; Z Zhang; E Doo; O Coux; A L Goldberg; T J Liang
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Journal:  J Virol       Date:  1998-11       Impact factor: 5.103

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3.  Expression patterns and action analysis of genes associated with hepatitis virus infection during rat liver regeneration.

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Review 7.  Impact of hepatitis B virus X protein on the DNA damage response during hepatocarcinogenesis.

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8.  Hepatitis B virus X protein and simian virus 5 V protein exhibit similar UV-DDB1 binding properties to mediate distinct activities.

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9.  Hepatitis B virus HBx protein localizes to mitochondria in primary rat hepatocytes and modulates mitochondrial membrane potential.

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10.  Proliferation defects and genome instability in cells lacking Cul4A.

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