AI Article Synopsis

  • The interaction between single-stranded DNA-binding proteins (SSBs) and the DNA replication machinery is crucial but not well understood, particularly in E. coli.
  • Researchers identified the binding site of SSB on the χ subunit of DNA polymerase III and explored the effects of disrupting this interaction.
  • The study finds that while the χ/SSB interaction is not essential for lagging-strand primer usage, it plays a significant role in stabilizing the replisome and ensuring coordinated DNA synthesis, with implications for cell cycle stability.

Article Abstract

Interactions between single-stranded DNA-binding proteins (SSBs) and the DNA replication machinery are found in all organisms, but the roles of these contacts remain poorly defined. In Escherichia coli, SSB's association with the χ subunit of the DNA polymerase III holoenzyme has been proposed to confer stability to the replisome and to aid delivery of primers to the lagging-strand DNA polymerase. Here, the SSB-binding site on χ is identified crystallographically and biochemical and cellular studies delineate the consequences of destabilizing the χ/SSB interface. An essential role for the χ/SSB interaction in lagging-strand primer utilization is not supported. However, sequence changes in χ that block complex formation with SSB lead to salt-dependent uncoupling of leading- and lagging-strand DNA synthesis and to a surprising obstruction of the leading-strand DNA polymerase in vitro, pointing to roles for the χ/SSB complex in replisome establishment and maintenance. Destabilization of the χ/SSB complex in vivo produces cells with temperature-dependent cell cycle defects that appear to arise from replisome instability.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3199393PMC
http://dx.doi.org/10.1038/emboj.2011.305DOI Listing

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