Acquisition of the rfb-gnd Cluster in Evolution of Escherichia coli O55 and O157

doi:10.1128/JB.182.21.6183-6191.2000

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Journal of Bacteriology, November 2000, p. 6183-6191, Vol. 182, No. 21
0021-9193/00/$04.00+0
Copyright © 2000, American Society for Microbiology. All rights reserved.

Acquisition of the rfb-gnd Cluster in Evolution of Escherichia coli O55 and O157

Phillip I. Tarr,¹^,²^,^* Laura M. Schoening,¹ Yoo-Lee Yea,¹ Teresa R. Ward,¹ Srdjan Jelacic,¹ and Thomas S. Whittam³

Children's Hospital and Regional Medical Center¹ and University of Washington School of Medicine,² Seattle, Washington 98105, and Pennsylvania State University, University Park, Pennsylvania 16802³

Received 30 December 1999/Accepted 7 July 2000

The rfb region specifies the structure of lipopolysaccharide side chains that comprise the diverse gram-negative bacterialsomatic (O) antigens. The rfb locus is adjacent to gnd, whichis a polymorphic gene encoding 6-phosphogluconate dehydrogenase.To determine if rfb and gnd cotransfer, we sequenced gnd in fiveO55 and 13 O157 strains of Escherichia coli. E. coli O157:H7 hasa gnd allele (allele A) that is only 82% identical to the gndallele (allele D) of closely related E. coli O55:H7. In contrast,gnd alleles of E. coli O55 in distant lineages are >99.9% identicalto gnd allele D. Though gnd alleles B and C in E. coli O157 thatare distantly related to E. coli O157:H7 are more similar to alleleA than to allele D, there are nucleotide differences at 4 to 6%of their sites. Alleles B and C can be found in E. coli O157 indifferent lineages, but we have found allele A only in E. coliO157 belonging to the DEC5 lineage. DNA 3' to the O55 gnd allelein diverse E. coli lineages has sequences homologous to tnpA ofthe Salmonella enterica serovar Typhimurium IS200 element, E.coli Rhs elements (including an H-rpt gene), and portions of theO111 and O157 rfb regions. We conclude that rfb and gnd cotransferredinto E. coli O55 and O157 in widely separated lineages and thatrecombination was responsible for recent antigenic shifts in theemergence of pathogenic E. coli O55 andO157.

^* Corresponding author. Mailing address: Division of Gastroenterology, MS: CH-24, Children's Hospital and Regional Medical Center,4800 Sand Point Way NE, Seattle, WA 98105. Phone: (206) 526-2521.Fax: (206) 528-2721. E-mail: tarr{at}u.washington.edu.

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