Comparison of Loss of Serum Resistance by Defined Lipopolysaccharide Mutants and an Acapsular Mutant of Uropathogenic Escherichia coli O75:K5

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Infection and Immunity, September 1998, p. 4244-4253, Vol. 66, No. 9
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

Comparison of Loss of Serum Resistance by Defined Lipopolysaccharide Mutants and an Acapsular Mutant of Uropathogenic Escherichia coli O75:K5

Stacy M. Burns,^* and Sheila I. Hull

Department of Microbiology and Immunology, Baylor College of Medicine, Houston, Texas 77030

Received 12 February 1998/Returned for modification 27 March 1998/Accepted 4 June 1998

In order to determine the importance of the O75 O antigen versus the K5 capsular antigen and the bimodal distribution of lipopolysaccharides(LPSs) in protection from complement-mediated lysis, mutants weremade by insertion of a cat or an aphA gene in or in place of genesnecessary for the synthesis of LPS and/or the K antigen of anO75⁺ K5⁺ uropathogenic Escherichia coli strain, GR-12. Mutations weremade in the following genes: the rfbD gene (required for the synthesisof TDP-rhamnose), the rfbKM genes (necessary for the synthesisof GDP-mannose), the rol gene (regulating O-antigen length), thekfiC gene (encoding a putative glycosyltransferase), and the kfiC-rfbDgenes. The resulting phenotypes were rough (O75), core plus one partial O-antigen subunit, random distributionof O-antigen chain lengths, acapsular (K5), and O75 K5, respectively. All five mutants and GR-12 were analyzed for survivalin 80% serum. The GR-12 parent was resistant, exhibiting a 500%increase in numbers. The rol, rfbKM, rfbD, and kfiC-rfbD mutantswere sensitive, experiencing 99%, 99.9%, 99.9%, and at least 99.999%killing, respectively, in the first hour. The kfiC mutant, however,increased in numbers in the first hour but experienced delayedsensitivity, decreasing in viability by 80% in the third hour.Single mutants were complemented with the wild-type gene in trans,showing restoration of the wild-type phenotype and serum resistance.Therefore, the O75 antigen is more important for survival in serumthan the K5 antigen, and regulation of the O75 O-antigen chainlength is crucial for protection of the bacteria from complement-mediatedlysis.

^* Corresponding author. Mailing address: Department of Microbiology and Immunology, Baylor College of Medicine, One Baylor Plaza,Houston, TX 77030. Phone: (713) 798-4021. Fax: (713) 798-7375.E-mail: sb691010{at}bcm.tmc.edu.

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