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. 2007 Jan;75(1):299-305.
doi: 10.1128/IAI.00952-06. Epub 2006 Nov 6.

A bile salt hydrolase of Brucella abortus contributes to the establishment of a successful infection through the oral route in mice

M Victoria Delpino  1 María I MarchesiniSilvia M EsteinDiego J ComerciJuliana CassataroCarlos A FossatiPablo C Baldi
Affiliations

A bile salt hydrolase of Brucella abortus contributes to the establishment of a successful infection through the oral route in mice

M Victoria Delpino et al. Infect Immun. 2007 Jan.

Abstract

Choloylglycine hydrolase (CGH), a bile salt hydrolase, has been annotated in all the available genomes of Brucella species. We obtained the Brucella CGH in recombinant form and demonstrated in vitro its capacity to cleave glycocholate into glycine and cholate. Brucella abortus 2308 (wild type) and its isogenic Deltacgh deletion mutant exhibited similar growth rates in tryptic soy broth in the absence of bile. In contrast, the growth of the Deltacgh mutant was notably impaired by both 5% and 10% bile. The bile resistance of the complemented mutant was similar to that of the wild-type strain. In mice infected through the intragastric or the intraperitoneal route, splenic infection was significantly lower at 10 and 20 days postinfection in animals infected with the Deltacgh mutant than in those infected with the wild-type strain VSports手机版. For both routes, no differences in spleen CFU were found between animals infected with the wild-type strain and those infected with the complemented mutant. Mice immunized intragastrically with recombinant CGH mixed with cholera toxin (CGH+CT) developed a specific mucosal humoral (immunoglobulin G [IgG] and IgA) and cellular (interleukin-2) immune responses. Fifteen days after challenge by the same route with live B. abortus 2308 cells, splenic CFU counts were 10-fold lower in mice immunized with CGH+CT than in mice immunized with CT or phosphate-buffered saline. This study shows that CGH confers on Brucella the ability to resist the antimicrobial action of bile salts. The results also suggest that CGH may contribute to the ability of Brucella to infect the host through the oral route. .

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Figures

FIG. 1.
FIG. 1.
In vitro cleavage of glycocholate by recombinant CGH. Released glycine was measured with the ninhydrin reaction. The same procedure was performed in the presence of mouse anti-CGH serum and normal mouse serum and in the absence of enzyme (to control for the spontaneous release of glycine).
FIG. 2.
FIG. 2.
Growth of B. abortus 2308 (WT), its isogenic Δcgh mutant (Δcgh), and the complemented mutant in TSB containing different concentrations of bile. Data indicate the number of viable bacteria at 18 h of culture in each medium in triplicate experiments.
FIG. 3.
FIG. 3.
Spleen colonization by B. abortus 2308 (WT), its isogenic Δcgh mutant (Δcgh), and the complemented mutant (comp) following oral (A) or intraperitoneal (B) infection of mice.**, significantly different medians (P = 0.0079, Mann-Whitney U test).
FIG. 4.
FIG. 4.
Antibody responses elicited in mice by oral immunization with CGH plus cholera toxin (adjuvant). Levels of specific anti-CGH antibodies were measured by ELISA in serum, saliva, and fecal extracts.
FIG. 5.
FIG. 5.
Specific in vitro production of IL-2 by cells obtained from spleens and mesenteric lymph nodes of mice immunized with CGH plus cholera toxin. Cells were stimulated with recombinant CGH, and IL-2 levels were measured 48 h later in culture supernatants.
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References

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