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- W2024792987 abstract "Structural comparisons between bacteriophage PRD1 and adenovirus have revealed an evolutionary relationship that has contributed significantly to current ideas on virus phylogeny. However, the structural organization of the receptor-binding spike complex and how the different symmetry mismatches are mediated between the spike-complex proteins are not clear. We determined the architecture of the PRD1 spike complex by using electron microscopy and three-dimensional image reconstruction of a series of PRD1 mutants. We constructed an atomic model for the full-length P5 spike protein by using comparative modeling. P5 was shown to be bound directly to the penton base protein P31. P5 and the receptor-binding protein P2 form two separate spikes, interacting with each other near the capsid shell. P5, with a tumor necrosis factor-like head domain, may have been responsible for host recognition before capture of the current receptor-binding protein P2." @default.
- W2024792987 created "2016-06-24" @default.
- W2024792987 creator A5026617852 @default.
- W2024792987 creator A5028590743 @default.
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- W2024792987 date "2007-04-17" @default.
- W2024792987 modified "2023-10-03" @default.
- W2024792987 title "Tale of two spikes in bacteriophage PRD1" @default.
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- W2024792987 doi "https://doi.org/10.1073/pnas.0608625104" @default.
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