cris.boxmetadata.label.title
Mechanism of force generation of a viral DNA packaging motor
cris.boxmetadata.label.dateissued
09 browse.startsWith.months.september 2005
cris.boxmetadata.label.accesslevel
open access
cris.boxmetadata.label.resourcetype
journal article
cris.boxmetadata.label.authors
Chemla Y.R.
Aathavan K.
Michaelis J.
Grimes S.
Jardine P.J.
Anderson D.L.
University of California
cris.boxmetadata.label.publisher
Elsevier B.V.
cris.boxmetadata.label.abstract
A large family of multimeric ATPases are involved in such diverse tasks as cell division, chromosome segregation, DNA recombination, strand separation, conjugation, and viral genome packaging. One such system is the Bacillus subtilis phage φ29 DNA packaging motor, which generates large forces to compact its genome into a small protein capsid. Here we use optical tweezers to study, at the single-molecule level, the mechanism of force generation in this motor. We determine the kinetic parameters of the packaging motor and their dependence on external load to show that DNA translocation does not occur during ATP binding but is likely triggered by phosphate release. We also show that the motor subunits act in a coordinated, successive fashion with high processivity. Finally, we propose a minimal mechanochemical cycle of this DNA-translocating ATPase that rationalizes all of our findings. Copyright ©2005 by Elsevier Inc.
cris.boxmetadata.label.citationstartpage
683
cris.boxmetadata.label.citationendpage
692
cris.boxmetadata.label.volume
122
cris.boxmetadata.label.issue
5
cris.boxmetadata.label.language
English
cris.boxmetadata.label.ocdeknowledgeArea
Bioquímica, Biología molecular
cris.boxmetadata.label.doi
cris.boxmetadata.label.scopusidentifier
2-s2.0-24144478521
cris.boxmetadata.label.pubmedidentifier
cris.boxmetadata.label.source
Cell
cris.boxmetadata.label.containerissn
0092009286748674
cris.boxmetadata.label.sponsor
We thank S.B. Smith, D.E. Smith, S.J. Tans, N.R. Forde, Z.D. Bryant, S. Dumont, J. Gore, J. Erzberger, J. Berger, O. Igoshin, J.-C. Liao, G. Oster, and L. Aravind for helpful discussion. This research was supported in part by grants from NIH GM-071552 (C.B.), NIH DE-03606 (D.L.A.), NIH GM-059604 (S.G.), DOE DE-AC03-76DF00098 (C.B.), and the Packard Foundation 1999-8325 (C.B.). Y.R.C. is supported by a National Research Service Award fellowship from NIH GM-65786 and a Career Award at the Scientific Interface from the Burroughs Wellcome Fund. K.A. is supported by the Program in Mathematics and Molecular Biology through a Burroughs Wellcome Fund fellowship.
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