Inactivation of DsbA, but Not DsbC and DsbD, Affects the Intracellular Survival and Virulence of Shigella flexneri

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Infect Immun, August 1998, p. 3909-3917, Vol. 66, No. 8
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

Inactivation of DsbA, but Not DsbC and DsbD, Affects the Intracellular Survival and Virulence of Shigella flexneri

Jun Yu^*

Molecular Infectious Diseases Group, Department of Paediatrics, Imperial College School of Medicine at St. Mary's, London W2 1PG, United Kingdom

Received 9 February 1998/Returned for modification 3 April 1998/Accepted 9 May 1998

In this study, three mutants, dsbA::kan, dsbC-kan, and dsbD-kan, of Shigella flexneri serotype 5 were constructed and characterizedto investigate the role of the periplasmic thiol:disulfide oxidoreductasesin pathogenicity. In gentamicin protection assays and the Serénytest, the dsbA mutant showed reduced virulence while the dsbCand dsbD mutants were similar to the wild type. That inactivationof dsbA was responsible for the reduced virulence was verifiedby complementation with the cloned wild-type gene in in vitroand in vivo assays. Despite the changed virulence behavior, thedsbA mutant could penetrate HeLa cells 15 min postinfection, consistentwith the fact that it actively secretes Ipa proteins upon Congored induction. Furthermore, the dsbA mutant was able to produceactin comets and protrusions, indicating its capacity for intra-and intercellular spread. However, a kinetic analysis of intracellulargrowth showed that the dsbA mutant barely grew in HeLa cells duringa 4-h infection whereas the wild type had a doubling time of 41min. Electron microscopy analysis revealed that dsbA mutant bacteriawere trapped in protrusion-derived vacuoles surrounded by doublemembranes, resembling an icsB mutant reported previously. Moreover,the trapped bacteria appeared to be lysed simultaneously withthe double membranes, resulting in characteristic empty vacuolesin the host cell cytosol. Thus, the attenuation mechanism fordsbA mutant appears to be more complicated than was previouslysuggested.

^* Mailing address: Molecular Infectious Diseases Group, Department of Paediatrics, Imperial College School of Medicine at St.Mary's, Norfolk Place, London W2 1PG, United Kingdom. Phone: 0171886 6340. Fax: 0171 886 6284. E-mail: jun.yu{at}ic.ac.uk.

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