Cell Cycle Parameters of Proteus Mirabilis: Interdependence of the Biosynthetic Cell Cycle and the Interdivision Cycle

Overview

Journal J Bacteriol

Publisher American Society for Microbiology

Specialty Microbiology

Date 1985 Nov 1

PMID 3902797

Citations 2

Authors

J Gmeiner

E Sarnow

K Milde

Affiliations

Soon will be listed here.

Abstract

We investigated the time periods of DNA replication, lateral cell wall extension, and septum formation within the cell cycle of Proteus mirabilis. Cells were cultivated under three different conditions, yielding interdivision times of approximately 55, 57, and 160 min, respectively. Synchrony was achieved by sucrose density gradient centrifugation. The time periods were estimated by division inhibition studies with cephalexin, mecillinam, and nalidixic acid. In addition, DNA replication was measured by thymidine incorporation, and murein biosynthesis was measured by incorporation of N-acetylglucosamine into sodium dodecyl sulfate-insoluble murein sacculi. At interdivision times of 55 to 57 min murein biosynthesis for reproduction of a unit cell lasted longer than the interdivision time itself, whereas DNA replication finished within 40 min. Surprisingly, inhibition of DNA replication by nalidixic acid did not inhibit the subsequent cell division but rather the one after that. Because P. mirabilis fails to express several reactions of the recA-dependent SOS functions known from Escherichia coli, the drug allowed us to determine which DNA replication period actually governed which cell division. Taken together, the results indicate that at an interdivision time of 55 to 57 min, the biosynthetic cell cycle of P. mirabilis lasts approximately 120 min. To achieve the observed interdivision time, it is necessary that two subsequent biosynthetic cell cycles be tightly interlocked. The implications of these findings for the regulation of the cell cycle are discussed.

Citing Articles

Rate and topography of peptidoglycan synthesis during cell division in Escherichia coli: concept of a leading edge.

Wientjes F, Nanninga N J Bacteriol. 1989; 171(6):3412-9.

PMID: 2656655 PMC: 210065. DOI: 10.1128/jb.171.6.3412-3419.1989.

Proteus mirabilis mutants defective in swarmer cell differentiation and multicellular behavior.

Belas R, Erskine D, Flaherty D J Bacteriol. 1991; 173(19):6279-88.

PMID: 1917860 PMC: 208381. DOI: 10.1128/jb.173.19.6279-6288.1991.

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