Genetics, Vol. 159, 1405-1414, December 2001, Copyright © 2001
Growth-Dependent DNA Breakage and Cell Death in a Gyrase Mutant of Salmonella
Eloi Garía,
Lionello Bossia, and
Nara Figueroa-Bossia
a Centre de Génétique Moléculaire, CNRS, 91198 Gif-sur-Yvette, France
Corresponding author:
Nara Figueroa-Bossi, Centre de Génétique Moléculaire, CNRS, 91198 Gif-sur-Yvette Cedex, France., figueroa{at}cgm.cnrs-gif.fr (E-mail)
Communicating editor: G. R. SMITH
A class of gyrase mutants of Salmonella enterica mimics the properties of bacteria exposed to quinolones. These mutants suffer spontaneous DNA breakage during normal growth and depend on recombinational repair for viability. Unlike quinolone-treated bacteria, however, they do not show accumulation of cleavable gyrase-DNA complexes. In recA or recB mutant backgrounds, the temperature-sensitive (ts) allele gyrA208 causes rapid cell death at 43°. Here, we isolated "suppressor-of-death" mutations, that is, secondary changes that allow a gyrA208 recB double mutant to survive a prolonged exposure to 43° and subsequently to form colonies at 28°. In most isolates, the secondary change was itself a ts mutation. Three ts alleles were mapped in genes coding for amino acyl tRNA synthetases (alaS, glnS, and lysS). Allele alaS216 completely abolished DNA breakage in a gyrA208 recA double mutant. Likewise, treating this mutant with chloramphenicol prevented death and DNA damage at 43°. Additional suppressors of gyrA208 lethality include rpoB mutations and, surprisingly, icd mutations inactivating isocitrate dehydrogenase. We postulate that the primary effect of the gyrase alteration is to hamper replication fork movement. Inhibiting DNA replication under conditions of continuing macromolecular synthesis ("unbalanced growth") activates a mechanism that causes DNA breakage and cell death, reminiscent of "thymineless" lethality.
