Affiliation:
1. Unité de Pathogénie Bactérienne des Muqueuses, Institut Pasteur, 75724 Paris Cedex 15, France
Abstract
ABSTRACT
We recently described a new afimbrial adhesin, AfaE-VIII, produced by animal strains associated with diarrhea and septicemia and by human isolates associated with extraintestinal infections. Here, we report that the
afa-8
operon, encoding AfaE-VIII adhesin, from the human blood isolate
Escherichia coli
AL862 is carried by a 61-kb genomic region with characteristics typical of a pathogenicity island (PAI), including a size larger than 10 kb, the presence of an integrase-encoding gene, the insertion into a tRNA locus (
pheR
), and the presence of a small direct repeat at each extremity. Moreover, the G+C content of the
afa-8
operon (46.4%) is lower than that of the
E. coli
K-12/MG1655 chromosome (50.8%). Within this PAI, designated PAI I
AL862
, we identified open reading frames able to code for products similar to proteins involved in sugar utilization. Four probes spanning these sequences hybridized with 74.3% of pathogenic
afa-8
-positive
E. coli
strains isolated from humans and animals, 25% of human pathogenic
afa-8
-negative
E. coli
strains, and only 8% of fecal strains (
P
= 0.05), indicating that these sequences are strongly associated with the
afa-8
operon and that this genetic association may define a PAI widely distributed among human and animal
afa-8
-positive strains. One of the distinctive features of this study is that
E. coli
AL862 also carries another
afa-8
-containing PAI (PAI II
AL862
), which appeared to be similar in size and genetic organization to PAI I
AL862
and was inserted into the
pheV
gene. We investigated the insertion sites of
afa-8
-containing PAI in human and bovine pathogenic
E. coli
strains and found that this PAI preferentially inserted into the
pheV
gene.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Cited by
60 articles.
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