Identification and characterization of two Campylobacter jejuni adhesins for cellular and mucous substrates.

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Infect Immun. 1986 July; 53(1): 141-148

Identification and characterization of two Campylobacter jejuni adhesins for cellular and mucous substrates.

E McSweegan and R I Walker

ABSTRACT

Campylobacter jejuni is able to colonize the human intestinalmucosa and cause disease. For this reason, it was importantto investigate mechanisms by which C. jejuni adheres to epithelialcells and intestinal mucus gel. All strains of C. jejuni usedwere able to adhere to INT 407 epithelial cells and mucus, buthigh adherence to one substrate did not necessarily indicatecomparable adherence to the other. The adherence of C. jejunito cells was inhibited partially by treating the bacterial cellswith proteases or glutaraldehyde or by adding a certain carbohydrate(fucose or mannose) to the medium. The flagellum of C. jejuniwas identified as a potential adhesin by comparing adherenceof flagellated and aflagellated variants. Shearing of the bacterialcells to remove the flagella reduced bacterial adhesion, whereasimmobilization of the flagellum with KCN increased adhesion.Purified flagella showed specific, fucose-resistant bindingto epithelial cells but not to intestinal mucus. The presenceof a second, nonproteinaceous adhesin was suggested becauseno single treatment of the bacteria completely inhibited adhesion.Lipopolysaccharide (LPS) was identified as another C. jejuniadhesin. [3H]LPS specifically bound to epithelial cells, andthis phenomenon was inhibited by periodate oxidation of theLPS or glutaraldehyde fixation of the epithelial cells. LPS,unlike flagella, was fucose sensitive and inhibited bindingof whole bacterial cells to INT 407 cells. LPS was also ableto bind to intestinal mucus gel. These data indicate that bothflagella and LPS are important in adhesion to the mucosal surface.

Infect Immun. 1986 July; 53(1): 141-148

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