AI Article Synopsis
- VP16 is a key protein in herpes simplex virus that activates the virus's immediate-early (IE) genes, with four new phosphorylation sites identified.
- The Ser375 site was studied after finding it mutated, resulting in a slower growth rate of the virus and reduced gene expression.
- The mutation also decreased the interaction between VP16 and the Oct-1 protein, suggesting that Ser375 is crucial for their cooperative binding to IE gene promoters.
Article Abstract
VP16 is a virion phosphoprotein of herpes simplex virus and a transcriptional activator of the viral immediate-early (IE) genes. We identified four novel VP16 phosphorylation sites (Ser18, Ser353, Ser411, and Ser452) at late times in infection but found no evidence of phosphorylation of Ser375, a residue reportedly phosphorylated when VP16 is expressed from a transfected plasmid. A virus carrying a Ser375Ala mutation of VP16 was viable in cell culture but with a slow growth rate. The association of the mutant VP16 protein with IE gene promoters and subsequent IE gene expression was markedly reduced during infection, consistent with prior transfection and in vitro results. Surprisingly, the association of Oct-1 with IE promoters was also diminished during infection by the mutant strain. We propose that Ser375 is important for the interaction of VP16 with Oct-1, and that the interaction is required to enable both proteins to bind to IE promoters.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1717022 | PMC |
| http://dx.doi.org/10.1016/j.virol.2005.10.011 | DOI Listing |
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