Cloning and sequencing of the genes encoding Escherichia coli cytolethal distending toxin.

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Infection and Immunity, January 1994, p. 244-251, Vol. 62, No. 1
0019-9567/1994/$04.00+0 DOI:

research-article

Cloning and sequencing of the genes encoding Escherichia coli cytolethal distending toxin.

D A Scott and J B Kaper

Department of Medicine, University of Maryland School of Medicine, Baltimore 21201.

ABSTRACT

Escherichia coli strains expressing cytolethal distending toxin(CDT) cause elongation of CHO cells at 24 h, followed by progressivecellular distention and death for up to 120 h. Similar distentionand cytotoxicity are seen in HeLa, HEp-2, and, to a lesser extent,Vero cells. The initial elongation in CHO cells is indistinguishablefrom that caused by E. coli heat-labile toxin (LT). In contrastto those from LT strains, supernatants from these strains haveno effect on Y-1 adrenal cells. TnphoA was introduced into CDT-positiveE. coli E6468/62 (O86:H34), isolated from a child with diarrhea,and 13 CDT-negative transconjugants were identified. DNA probesconstructed from DNA flanking the TnphoA insertion sites ofCDT-negative mutants were used to identify a CDT-positive clonefrom an E6468/62 genomic library with a 5.5-kb insert. Exonucleasedeletions were created and assayed in CHO cells. In this manner,a 2.3-kb CDT-active region was defined, and the nucleotide sequencewas determined. Sequence analysis identified three open readingframes (ORFs), designated cdtA, cdtB, and cdtC. These contain711, 819, and 570 bp, respectively, and encode polypeptideswith predicted molecular masses of 25.5, 29.8, and 20.3 kDa,respectively. Each ORF has a putative signal sequence, and thereare 4-bp overlaps between cdtA and cdtB and between cdtB andcdtC. The nucleotide and predicted amino acid sequences haveno significant homology with those of any previously reportedgenes or proteins. By in vitro transcription-translation andan anti-alkaline phosphatase immunoblot, native proteins and/orfusion proteins corresponding to each ORF were identified.

Infection and Immunity, January 1994, p. 244-251, Vol. 62, No. 1
0019-9567/1994/$04.00+0 DOI:

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