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The Replicative DnaE Polymerase of Bacillus subtilis Recruits the Glycolytic Pyruvate Kinase (PykA) When Bound to Primed DNA Templates

Alexandria Holland, Matthaios Pitoulias, Panos Soultanas, Laurent Janniere

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Abstract

The glycolytic enzyme PykA has been reported to drive the metabolic control of replication through a mechanism involving PykA moonlighting functions on the essential DnaE polymerase, the DnaC helicase and regulatory determinants of PykA catalytic activity in Bacillus subtilis. The mutants of this control suffer from critical replication and cell cycle defects, showing that the metabolic control of replication plays important functions in the overall rate of replication. Using biochemical approaches, we demonstrate here that PykA interacts with DnaE for modulating its activity when the replication enzyme is bound to a primed DNA template. This interaction is mediated by the CAT domain of PykA and possibly allosterically regulated by its PEPut domain, which also operates as a potent regulator of PykA catalytic activity. Furthermore, using fluorescence microscopy we show that the CAT and PEPut domains are important for the spatial localization of origins and replication forks, independently of their function in PykA catalytic activity. Collectively, our data suggest that the metabolic control of replication depends on the recruitment of PykA by DnaE at sites of DNA synthesis. This recruitment is likely highly dynamic, as DnaE is frequently recruited to and released from replication machineries to extend the several thousand RNA primers generated from replication initiation to termination. This implies that PykA and DnaE continuously associate and dissociate at replication machineries for ensuring a highly dynamic coordination of the replication rate with metabolism.

Original languageEnglish
Article number965
Number of pages17
JournalLife
Volume13
Issue number4
Early online date6 Apr 2023
DOIs
Publication statusPublished - 7 Apr 2023

Bibliographical note

Publisher Copyright:
© 2023 by the authors.

Data Availability Statement

All data are contained within the article.

Funding

This work was supported by a Biotechnology Biological Sciences Research Council (BBSRC) grant: BB/R013357/1 to P.S., a University of Nottingham sub-contract RIS1165589 to L.J., and by recurring research funds from CNRS (Centre National de la Recherche Scientifique) and UEVE (Univesité d’Evry Val d’Essonne) to L.J. M.P. was partially supported by a University of Nottingham Vice Chancellor’s Excellence PhD award.

Keywords

  • DnaE
  • metabolism
  • microbiology
  • moonlighting activity
  • PykA
  • replication

ASJC Scopus subject areas

  • Ecology, Evolution, Behavior and Systematics
  • General Biochemistry,Genetics and Molecular Biology
  • Space and Planetary Science
  • Palaeontology

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