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The Synchronization of Replication and Division Cycles in Individual E. coli Cells

Isogenic E. coli cells growing in a constant environment display significant variability in growth rates, division sizes, and generation times. The guiding principle appears to be that each cell, during one generation, adds a size increment that is uncorrelated to its birth size. Here, we investigat...

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Bibliographic Details
Published in:Cell 2016-07, Vol.166 (3), p.729-739
Main Authors: Wallden, Mats, Fange, David, Lundius, Ebba Gregorsson, Baltekin, Özden, Elf, Johan
Format: Article
Language:English
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Summary:Isogenic E. coli cells growing in a constant environment display significant variability in growth rates, division sizes, and generation times. The guiding principle appears to be that each cell, during one generation, adds a size increment that is uncorrelated to its birth size. Here, we investigate the mechanisms underlying this “adder” behavior by mapping the chromosome replication cycle to the division cycle of individual cells using fluorescence microscopy. We have found that initiation of chromosome replication is triggered at a fixed volume per chromosome independent of a cell’s birth volume and growth rate. Each initiation event is coupled to a division event after a growth-rate-dependent time. We formalize our findings in a model showing that cell-to-cell variation in division timing and cell size is mainly driven by variations in growth rate. The model also explains why fast-growing cells display adder behavior and correctly predict deviations from the adder behavior at slow growth. [Display omitted] •Replication initiates at a nearly fixed volume per chromosome for all growth rates•The time from initiation to division depends on the individual cell’s growth rate•Variation in growth rate sets the variation in generation time and division size•E. coli appears as a “sizer” at slow growth and an “adder” at fast growth Cell-to-cell variation in division timing and cell size in E. coli is due to differences in growth rate, whereas the timing of replication is triggered at an invariant fixed volume per chromosome.
ISSN:0092-8674
1097-4172
1097-4172
DOI:10.1016/j.cell.2016.06.052