| Literature DB >> 32149608 |
Matthieu Bergé1, Julian Pezzatti2, Víctor González-Ruiz2,3, Laurence Degeorges1, Geneviève Mottet-Osman1, Serge Rudaz2,3, Patrick H Viollier1.
Abstract
Proliferating cells must coordinate central metabolism with the cell cycle. How central energy metabolism regulates bacterial cell cycle functions is not well understood. Our forward genetic selection unearthed the Krebs cycle enzyme citrate synthase (CitA) as a checkpoint regulator controlling the G1→S transition in the polarized alpha-proteobacterium Caulobacter crescentus, a model for cell cycle regulation and asymmetric cell division. We find that loss of CitA promotes the accumulation of active CtrA, an essential cell cycle transcriptional regulator that maintains cells in G1-phase, provided that the (p)ppGpp alarmone is present. The enzymatic activity of CitA is dispensable for CtrA control, and functional citrate synthase paralogs cannot replace CitA in promoting S-phase entry. Our evidence suggests that CitA was appropriated specifically to function as a moonlighting enzyme to link central energy metabolism with S-phase entry. Control of the G1-phase by a central metabolic enzyme may be a common mechanism of cellular regulation.Entities:
Keywords: (p)ppGpp; Caulobacter crescentus; TCA cycle; cell biology; cell development; citrate synthase; infectious disease; microbiology; moonlighting enzyme
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Year: 2020 PMID: 32149608 PMCID: PMC7083601 DOI: 10.7554/eLife.52272
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140