Minor proteins, mobile arms and membrane–capsid interactions in the bacteriophage PRD1 capsid

被引:0
|
作者
Carmen San Martín
Juha T. Huiskonen
Jaana K. H. Bamford
Sarah J. Butcher
Stephen D. Fuller
Dennis H. Bamford
Roger M. Burnett
机构
[1] The Wistar Institute,Department of Biosciences and Institute of Biotechnology
[2] Viikki Biocenter,The Division of Structural Biology
[3] University of Helsinki,undefined
[4] Wellcome Trust Centre for Human Genetics,undefined
[5] The Henry Wellcome Building for Genomic Medicine,undefined
[6] University of Oxford,undefined
来源
Nature Structural Biology | 2002年 / 9卷
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摘要
Bacteriophage PRD1 shares many structural and functional similarities with adenovirus. A major difference is the PRD1 internal membrane, which acts in concert with vertex proteins to translocate the phage genome into the host. Multiresolution models of the PRD1 capsid, together with genetic analyses, provide fine details of the molecular interactions associated with particle stability and membrane dynamics. The N- and C-termini of the major coat protein (P3), which are required for capsid assembly, act as conformational switches bridging capsid to membrane and linking P3 trimers. Electrostatic P3–membrane interactions increase virion stability upon DNA packaging. Newly revealed proteins suggest how the metastable vertex works and how the capsid edges are stabilized.
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页码:756 / 763
页数:7
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