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Differential functional behavior of viral phi29, Nf and GA-1 SSB proteins
Authors:Gascón I  Lázaro J M  Salas M
Affiliation:Irene Gascón, José M. Lázaro, and Margarita Salas
Abstract:DNA replication of [var phi]29 and related phages takes place via a strand displacement mechanism, a process that generates large amounts of single-stranded DNA (ssDNA). Consequently, phage-encoded ssDNA-binding proteins (SSBs) are essential proteins during phage [var phi]29-like DNA replication. In the present work we analyze the helix-destabilizing activity of the SSBs of [var phi]29 and the related phages Nf and GA-1, their ability to eliminate non-productive binding of [var phi]29 DNA polymerase to ssDNA and their stimulatory effect on replication by [var phi]29 DNA polymerase in primed M13 ssDNA replication, a situation that resembles type II replicative intermediates that occur during [var phi]29-like DNA replication. Significant differences have been appreciated in the functional behavior of the three SSBs. First, the GA-1 SSB is able to display helix-destabilizing activity and to stimulate dNTP incorporation by [var phi]29 DNA polymerase in the M13 DNA replication assay, even at SSB concentrations at which the [var phi]29 and Nf SSBs do not show any effect. On the other hand, the [var phi]29 SSB is the only one of the three SSBs able to increase the replication rate of [var phi]29 DNA polymerase in primed M13 ssDNA replication. From the fact that the [var phi]29 SSB, but not the Nf SSB, stimulates the replication rate of Nf DNA polymerase we conclude that the different behaviors of the SSBs on stimulation of the replication rate of [var phi]29 and Nf DNA polymerases is most likely due to formation of different nucleoprotein complexes of the SSBs with the ssDNA rather than to a specific interaction between the SSB and the corresponding DNA polymerase. A model that correlates the thermodynamic parameters that define SSB–ssDNA nucleoprotein complex formation with the functional stimulatory effect of the SSB on [var phi]29-like DNA replication has been proposed.
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