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Atomistic basis of force generation, translocation, and coordination in a viral genome packaging motor
Author(s) -
Joshua Pajak,
Erik Dill,
Emilio Reyes-Aldrete,
Mark A. White,
Brian A. Kelch,
Paul J. Jardine,
Gaurav Arya,
Marc C. Morais
Publication year - 2021
Publication title -
nucleic acids research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 9.008
H-Index - 537
eISSN - 1362-4954
pISSN - 0305-1048
DOI - 10.1093/nar/gkab372
Subject(s) - dna , biophysics , biology , capsid , molecular motor , atpase , protein subunit , atp hydrolysis , helix (gastropod) , molecular dynamics , planar , genome , crystallography , biochemistry , genetics , enzyme , chemistry , virus , computational chemistry , gene , ecology , computer graphics (images) , snail , computer science
Double-stranded DNA viruses package their genomes into pre-assembled capsids using virally-encoded ASCE ATPase ring motors. We present the first atomic-resolution crystal structure of a multimeric ring form of a viral dsDNA packaging motor, the ATPase of the asccφ28 phage, and characterize its atomic-level dynamics via long timescale molecular dynamics simulations. Based on these results, and previous single-molecule data and cryo-EM reconstruction of the homologous φ29 motor, we propose an overall packaging model that is driven by helical-to-planar transitions of the ring motor. These transitions are coordinated by inter-subunit interactions that regulate catalytic and force-generating events. Stepwise ATP binding to individual subunits increase their affinity for the helical DNA phosphate backbone, resulting in distortion away from the planar ring towards a helical configuration, inducing mechanical strain. Subsequent sequential hydrolysis events alleviate the accumulated mechanical strain, allowing a stepwise return of the motor to the planar conformation, translocating DNA in the process. This type of helical-to-planar mechanism could serve as a general framework for ring ATPases.

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