Rifaximin prophylaxis reduced risk of developing TD versus placeb

Rifaximin prophylaxis reduced risk of developing TD versus placebo (p < 0.0001). A smaller percentage of individuals who received rifaximin

versus placebo developed all-cause TD (20% vs 48%, respectively; p < 0.0001) or TD requiring antibiotic therapy (14% vs 32%, respectively; p = 0.003). More individuals in the rifaximin group (76%) completed treatment without developing TD versus those in the placebo group (51%; p = 0.0004). Rifaximin provided a 58% protection rate against TD and was associated with fewer adverse events than PF-562271 cost placebo. Conclusions. Prophylactic treatment with rifaximin 600 mg/d for 14 days safely and effectively reduced the risk of developing TD in US travelers to Mexico. Rifaximin chemoprevention should be considered

for TD in appropriate individuals traveling to high-risk regions. An estimated 40% of the 50 million individuals traveling from industrialized to developing countries each year develop travelers’ diarrhea (TD).1 This acute infectious 3-deazaneplanocin A solubility dmso illness is characterized by the passage of 7 to 13 watery stools over 2 days, accompanied by one or more additional enteric symptom.1,2 Based on microbiologic evaluation, enteric bacterial pathogens are thought to cause approximately 80% of TD cases, with strains of enterotoxigenic Escherichia coli (ETEC) and enteroaggregative E coli (EAEC) responsible for the majority of cases.3–5 Invasive bacterial pathogens including Shigella and Campylobacter contribute to approximately 4% to 20% of TD cases.5–7 Although TD is often self-limiting, lasting on average for 4 days, the negative consequences of acquiring this illness can be substantial, including disruption of travel plans and increased risk for development of postinfectious

complications,8 such as postinfectious irritable bowel syndrome (PI-IBS)9–14 and inflammatory bowel disease (IBD).15 Antibiotic chemoprophylaxis provides substantial protection from TD and prevents potentially severe complications.16 However, the guidelines recommended by the National Institutes of Health consensus panel in 1985 discouraged the routine administration of systemic antibiotics as ID-8 chemoprophylaxis for TD because of the potential adverse effects associated with administration and concern that overprescribing could contribute to the growing epidemic of antibiotic resistance.17 The ideal chemoprevention agent would achieve the efficacy of systemic antibiotics without the potential adverse effects and antibiotic resistance associated with these agents. Rifaximin (Xifaxan®; Salix Pharmaceuticals, Inc., Morrisville, NC, USA) is a gut-selective, nonsystemic antibiotic18 that has a low risk for development of clinically relevant antibiotic resistance.19 It is indicated for the treatment of TD caused by noninvasive strains of E coli2 and has demonstrated efficacy in treating TD in clinical studies.

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