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Published April 2018 | Published
Journal Article Open

Two-Stage Dynamics of In Vivo Bacteriophage Genome Ejection

Abstract

Biopolymer translocation is a key step in viral infection processes. The transfer of information-encoding genomes allows viruses to reprogram the cell fate of their hosts. Constituting 96% of all known bacterial viruses [A. Fokine and M. G. Rossmann, Molecular architecture of tailed double-stranded DNA phages, Bacteriophage 4, e28281 (2014)], the tailed bacteriophages deliver their DNA into host cells via an "ejection" process, leaving their protein shells outside of the bacteria; a similar scenario occurs for mammalian viruses like herpes, where the DNA genome is ejected into the nucleus of host cells, while the viral capsid remains bound outside to a nuclear-pore complex. In light of previous experimental measurements of in vivo bacteriophage λ ejection, we analyze here the physical processes that give rise to the observed dynamics. We propose that, after an initial phase driven by self-repulsion of DNA in the capsid, the ejection is driven by anomalous diffusion of phage DNA in the crowded bacterial cytoplasm. We expect that this two-step mechanism is general for phages that operate by pressure-driven ejection, and we discuss predictions of our theory to be tested in future experiments.

Additional Information

© 2018 The Author(s). Published by the American Physical Society under the terms of the Creative Commons Attribution 4.0 International license. Further distribution of this work must maintain attribution to the author(s) and the published article's title, journal citation, and DOI. (Received 1 July 2017; revised manuscript received 27 January 2018; published 1 May 2018) We are grateful to William Klug, David Van Valen, Mattias Rydenfelt, Arbel Tadmor, Ian Molineux, Maja Bialecka-Fornal, Heun Jin Lee, Timur Zhiyentayev, Long Cai, Stephanie Weber, Andrew Spakowitz, and Julie Theriot for helpful insights and discussions. This work was supported by La Fondation Pierre-Gilles de Gennes, the Rosen Center at Caltech, the James S. McDonnell Foundation, the National Institutes of Health DP1 OD000217 (Directors Pioneer Award), R01 GM085286 and 1R35 GM118043-01 (MIRA), F32 HL134288, the National Science Foundation Grants No. 1161803 and No. CHE1051507, and the Netherlands Organization for Scientific Research (NWO TOPGO grant).

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