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      Regulation of alphaherpesvirus infections by the ICP0 family of proteins.

      1 , 1
      The Journal of general virology
      Microbiology Society

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          Abstract

          Immediate-early protein ICP0 of herpes simplex virus type 1 (HSV-1) is important for the regulation of lytic and latent viral infection. Like the related proteins expressed by other alphaherpesviruses, ICP0 has a zinc-stabilized RING finger domain that confers E3 ubiquitin ligase activity. This domain is essential for the core functions of ICP0 and its activity leads to the degradation of a number of cellular proteins, some of which are involved in cellular defences that restrict viral infection. The article reviews recent advances in ICP0-related research, with an emphasis on the mechanisms by which ICP0 and related proteins counteract antiviral restriction and the roles in this process of cellular nuclear substructures known as ND10 or PML nuclear bodies. We also summarize recent advances in the understanding of the biochemical aspects of ICP0 activity. These studies highlight the importance of the SUMO conjugation pathway in both intrinsic resistance to HSV-1 infection and in substrate targeting by ICP0. The topics discussed in this review are relevant not only to HSV-1 infection, but also to cellular intrinsic resistance against herpesviruses more generally and the mechanisms by which viruses can evade this restriction.

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          Author and article information

          Journal
          J Gen Virol
          The Journal of general virology
          Microbiology Society
          1465-2099
          0022-1317
          Mar 2013
          : 94
          : Pt 3
          Affiliations
          [1 ] MRC-University of Glasgow Centre for Virus Research, 8 Church Street, Glasgow G11 5JR, Scotland, UK.
          Article
          10.1099/vir.0.048900-0
          23239572
          60801774-ef93-44de-a070-5b7eb962e8d0
          History

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