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Recent
Articles
Haijema BJ, Hahn J, Haynes J, Dubnau D.
A ComGA-dependent checkpoint limits growth during the escape
from competence.
Mol Microbiol 2001 Apr;40(1):52-64
PMID: 11298275
In Bacillus subtilis, competence for transformation develops in
5-10% of the cells in a stationary phase culture. These cells exhibit
a prolonged lag in the resumption of growth and cell division during
the escape from competence. To better understand the basis of this
lag, we have characterized competent cultures microscopically. To
distinguish the minority of competent cells, a translational fusion
between ComK, the competence transcription factor, and the green
fluorescent protein (GFP) was used as a marker. Only 5-10% of the
cells in a competent culture were fluorescent, indicating that ComK
synthesis is an all or nothing event. To validate the identification
of competent cells, we demonstrated the coincident expression of
comEA, a late competence gene, and comK-gfp. Competent cells resemble
stationary phase cells; the majority are single (not in chains),
contain single nucleoids, and rarely contain FtsZ rings. Upon dilution
into fresh medium, competent cells maintain this appearance for
about 2 h. In contrast, the majority of non-competent cells rapidly
resume growth, exhibiting chaining, nuclear division and FtsZ-ring
formation. The late competence protein ComGA is required for the
competence-related block in chromosome replication and cell division.
In the competent cells of a comGA mutant culture, chromosomal replication
and FtsZ-ring formation were no longer blocked, although competent
comGA mutant cells were abnormal in appearance. It is likely that
one role for ComGA is to prevent growth, chromosome replication
and cell division until ComK can be eliminated by degradation. A
mutation in the ATP-binding site of comGA inactivated the protein
for transformation but did not prevent it from inhibiting DNA replication
and cell division. The buoyant density difference between competent
and non-competent cells depends on the competence-specific growth
arrest.

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