Exploring Changes in the Host Gut Microbiota During a Controlled Human Infection Model for Campylobacter jejuni
Campylobacter jejuni infection is a leading cause of foodborne disease, common to children, adult travelers, and military populations in low- to middle-income countries. In the absence of a licensed vaccine, efforts to evaluate prophylactic agents are underway. The prophylactic efficacy of a twice-d...
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Veröffentlicht in: | Frontiers in cellular and infection microbiology 2021-08, Vol.11, p.702047-702047 |
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Sprache: | eng |
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Zusammenfassung: | Campylobacter jejuni
infection is a leading cause of foodborne disease, common to children, adult travelers, and military populations in low- to middle-income countries. In the absence of a licensed vaccine, efforts to evaluate prophylactic agents are underway. The prophylactic efficacy of a twice-daily, 550 mg dose of the antibiotic rifaximin demonstrated no efficacy against campylobacteriosis in a controlled human infection model (CHIM); however, samples from the CHIM study were utilized to assess how the human gut microbiome responds to
C. jejuni
infection, and if a ‘protective’ microbiota exists in study participants not developing campylobacteriosis. Statistically significant, but minor, differences in study participant beta diversity were identified during the challenge period (p = 0.002, R
2
= 0.042), but no significant differences were otherwise observed. Pre-challenge alpha diversity was elevated in study participants who did not develop campylobacteriosis compared to those who did (p < 0.001), but alpha diversity declined in all study participants from the pre-challenge period to post-discharge. Our work provides insight into gut microbiome shifts observed during a
C. jejuni
CHIM and following antibiotic treatment. This study utilized a high dose of 1.7 x 10
5
colony-forming units of
C. jejuni
; future work could include CHIM studies performed with inocula more closely mimicking natural exposure as well as field studies involving naturally-occurring enteric infections. |
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ISSN: | 2235-2988 2235-2988 |
DOI: | 10.3389/fcimb.2021.702047 |