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Multiple mechanisms for overcoming lethal over-initiation of DNA replication. | LitMetric

AI Article Synopsis

  • - DNA replication in bacteria is tightly regulated, with key players being the DnaA protein and the oriC region, as disturbances in replication can harm the cell's fitness.
  • - In a study of Bacillus subtilis, removing yabA, a regulator of replication initiation, created lethal conditions when paired with a mutation causing over-initiation, but several suppressor mutations were identified that restored cell viability.
  • - These suppressor mutations either promoted replication elongation or reduced initiation by lowering levels of the DnaC helicase, which is essential for starting replication, demonstrating the complexity of replication regulation in cells.

Article Abstract

DNA replication is highly regulated and primarily controlled at the step of initiation. In bacteria, the replication initiator DnaA and the origin of replication oriC are the primary targets of regulation. Perturbations that increase or decrease replication initiation can cause a decrease in cell fitness. We found that multiple mechanisms, including an increase in replication elongation and a decrease in replication initiation, can compensate for lethal over-initiation. We found that in Bacillus subtilis, under conditions of rapid growth, loss of yabA, a negative regulator of replication initiation, caused a synthetic lethal phenotype when combined with the dnaA1 mutation that also causes replication over-initiation. We isolated several classes of suppressors that restored viability to dnaA1 ∆yabA double mutants. Some suppressors (relA, nrdR) stimulated replication elongation. Others (dnaC, cshA) caused a decrease in replication initiation. One class of suppressors decreased replication initiation in the dnaA1 ∆yabA mutant by causing a decrease in the amount of the replicative helicase, DnaC. We found that decreased levels of helicase in otherwise wild-type cells were sufficient to decrease replication initiation during rapid growth, indicating that the replicative helicase is limiting for replication initiation. Our results highlight the multiple mechanisms cells use to regulate DNA replication.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9825946PMC
http://dx.doi.org/10.1111/mmi.14976DOI Listing

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