AI Article Synopsis

  • Proper assembly of viruses involves specific interactions between capsid proteins, with scaffolding proteins aiding in the formation of icosahedral capsids.
  • The study focuses on the bacteriophage P22's scaffolding protein, which mainly consists of helical structures and directs assembly through its C-terminal helix-turn-helix (HTH) domain binding to coat proteins.
  • Through alanine scanning mutagenesis, researchers identified that residues R293 and K296 in the scaffolding protein are essential for binding to the coat protein, while other neighboring charged amino acids influence the strength of this interaction.

Article Abstract

Proper assembly of viruses must occur through specific interactions between capsid proteins. Many double-stranded DNA viruses and bacteriophages require internal scaffolding proteins to assemble their coat proteins into icosahedral capsids. The 303 amino acid bacteriophage P22 scaffolding protein is mostly helical, and its C-terminal helix-turn-helix (HTH) domain binds to the coat protein during virion assembly, directing the formation of an intermediate structure called the procapsid. The interaction between coat and scaffolding protein HTH domain is electrostatic, but the amino acids that form the protein-protein interface have yet to be described. In the present study, we used alanine scanning mutagenesis of charged surface residues of the C-terminal HTH domain of scaffolding protein. We have determined that P22 scaffolding protein residues R293 and K296 are crucial for binding to coat protein and that the neighboring charges are not essential but do modulate the affinity between the two proteins.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3208733PMC
http://dx.doi.org/10.1016/j.virol.2011.09.005DOI Listing

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