Ability of Proteus mirabilis to invade human urothelial cells is coupled to motility and swarming differentiation.

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Infect Immun. 1992 November; 60(11): 4740-4746

Ability of Proteus mirabilis to invade human urothelial cells is coupled to motility and swarming differentiation.

C Allison, N Coleman, P L Jones and C Hughes

Department of Pathology, Cambridge University, United Kingdom.

ABSTRACT

Proteus mirabilis causes serious kidney infections which caninvolve invasion of host urothelial cells. We present data showingthat the ability to invade host urothelial cells is closelycoupled to swarming, a form of cyclical multicellular behaviorin which vegetative bacteria differentiate into hyperflagellated,filamentous swarm cells capable of coordinated and rapid populationmigration. Entry into the human urothelial cell line EJ/28 byP. mirabilis U6450 isolated at different stages throughout theswarming cycle was measured by the antibiotic protection assaymethod and confirmed by electron microscopy. Differentiatedfilaments entered urothelial cells within 30 min and were 15-foldmore invasive (ca. 0.18% entry in 2 h) than an equivalent dryweight of vegetative cells isolated before differentiation,which attained only ca. 0.012% entry in the 2-h assay. The invasiveability of P. mirabilis was modulated in parallel with flagellinlevels throughout two cycles of swarming. Septation and divisionof intracellular swarm cells produced between 50 and 300 vegetativebacteria per human cell, compared with 4 to 12 intracellularbacteria after incubation with vegetative cells. Transposon(Tn5) mutants of P. mirabilis with specific defects in motilityand multicellular behavior were compared with the wild-typefor the ability to invade. Mutants which lacked flagella (nonmotilenonswarming) were entirely noninvasive, and those which weremotile but defective in swarm cell formation (motile nonswarming)were 25-fold less invasive than wild-type vegetative cells.Mutants with defects in the coordination of multicellular migrationand the temporal control of consolidation (cyclical reversionof swarm cells to vegetative cells) were reduced ca. 3- to 12-foldin the ability to enter urothelial cells. In contrast, a nonhemolytictransposon mutant which swarmed normally retained over 80% ofwild-type invasive ability. Swarm cells and early consolidationcells were at least 10-fold more cytolytic than vegetative cellsas a result of their high-level production of hemolysin.

Infect Immun. 1992 November; 60(11): 4740-4746

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