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Chemotaxis plays multiple roles during Helicobacter pylori animal infection K Terry S M. Williams L Connolly K M. Ottemann, University of California, Santa Cruz
ABSTRACT: Helicobacter pylori is a human gastric pathogen associated with
gastric and duodenal ulcers as well as specific gastric cancers. H. pylori
infects approximately 50% of the world's population. and infections can persist
throughout the lifetime of the host. Motility and chemotaxis have been shown to
be important in the infection process of H. pylori. We sought to address the
specific roles of chemotaxis in infection of a mouse model system. We found
that mutants lacking cheW, cheA, or cheY are all nonchemotactic and infect
FVB/N mice with an attenuated phenotype after 2 weeks of infection. If
infections proceeded for 6 months, however, this attenuation disappeared.
Histological and culture analysis revealed that nonchemotactic mutants were
found only in the corpus of the stomach, while the wild type occupied both the
corpus and the antrum. Further analysis showed that nonchemotactic H. pylori
isolates had an increased 50% infectious dose and were greatly outcompeted when
coinfected with the wild type. If nonchemotactic mutants were allowed to
establish an infection, subsequent infection with the wild type partially
displaced the nonchemotactic mutants. indicating a role for chernotaxis in
maintenance of infection. he data presented here support four roles for
chemotaxis in H. pylori mouse infections: (i) establishing infection. (ii)
achieving high-level infection, (iii) maintaining an infection when there are
competing H. pylori present. and (iv) colonizing all regions of the
stomach.
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