AI Article Synopsis

  • HSV-1 capsids are assembled in the nucleus and gain their envelope and tegument before becoming infective, with the process involving both the inner and outer nuclear membranes.
  • Although Us3 aids in moving capsids from the nucleus to the cytoplasm, it's not vital for producing infectious viruses.
  • The study found that a strain lacking Us3 (R7041(∆US3)) had more capsids and virions in the perinuclear space and produced a larger number of viral particles compared to wild type HSV-1 within 24 hours post-infection.

Article Abstract

Herpes simplex virus 1 (HSV-1) capsids are assembled in the nucleus bud at the inner nuclear membrane into the perinuclear space, acquiring envelope and tegument. In theory, these virions are de-enveloped by fusion of the envelope with the outer nuclear membrane and re-enveloped by Golgi membranes to become infective. Us3 enables the nucleus to cytoplasm capsid translocation. Nevertheless, Us3 is not essential for the production of infective progeny viruses. Determination of phenotype distribution by quantitative electron microscopy, and calculation per mean nuclear or cell volume revealed the following: (i) The number of R7041(∆US3) capsids budding at the inner nuclear membrane was significantly higher than that of wild type HSV-1; (ii) The mean number of R7041(∆US3) virions per mean cell volume was 2726, that of HSV-1 virions 1460 by 24 h post inoculation; (iii) 98% of R7041(∆US3) virions were in the perinuclear space; (iv) The number of R7041(∆US3) capsids in the cytoplasm, including those budding at Golgi membranes, was significantly reduced. Cell associated R7041(∆US3) yields were 2.37×10(8) and HSV-1 yields 1.57×10(8) PFU/mL by 24 h post inoculation. We thus conclude that R7041(∆US3) virions, which acquire envelope and tegument by budding at the inner nuclear membrane into the perinuclear space, are infective.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4306828PMC
http://dx.doi.org/10.3390/v7010052DOI Listing

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