In medical practice,
antibiotics are generally given empirically for the treatment of acute exacerbations of
chronic bronchitis (AECB). To be effective,
antibiotic therapy should be broad in spectrum, and it should also cover the common
beta-lactamase-producing pathogens. In this multicenter, randomized, investigator-masked study, 469 patients with AECB were randomized (in a ratio of 2:1) to receive 400-mg oral
ceftibuten capsules once daily or 500-mg
amoxicillin-
clavulanate tablets three times daily for 5 to 15 days. Patients receiving
ceftibuten were further divided into those who took the
capsule with a meal (fed) and those who took the
capsule 1 hour before a meal (fasted). Clinical and microbiologic responses were evaluated
after treatment at 0 to 6 days (end of treatment) and 7 to 21 days (follow-up). Overall clinical success was determined by cure/improvement of signs and symptoms of AECB at the end of treatment and at follow-up. Overall microbiologic assessment was graded as eradication, persistence, relapse,
reinfection, colonization,
superinfection, or unassessable. Tolerability was evaluated by grading observed adverse events. The mean
duration of treatment was 10.4 days for patients who received
ceftibuten and 10.1 days for patients who received
amoxicillin-
clavulanate. A total of 252 patients receiving
ceftibuten and 117 patients receiving
amoxicillin-
clavulanate were evaluable for clinical efficacy, and 55 patients were evaluable for microbiologic response. Both treatments improved the signs and symptoms of
bronchitis, and overall clinical success rates were equivalent for patients treated with
ceftibuten (211 of 252 [84%]) and
amoxicillin-
clavulanate (93 of 117 [79%]) (95% confidence interval [CI], -4.5% to 13.6%). Overall microbiologic eradication rates were also similar for patients treated with
ceftibuten (36 of 37 [97%]) and
amoxicillin-
clavulanate (12 of 14 [86%]) (95% CI, -5.2% to 21.2%). The most frequently reported treatment-related adverse events were gastrointestinal disturbances, which occurred in 15% (47 of 316) and 24% (36 of 152) of patients treated with
ceftibuten and
amoxicillin-
clavulanate, respectively. No significant difference was observed in the ceftibutenfed and
ceftibuten-fasted groups in overall clinical assessments of the clinical efficacy population and safety population. In conclusion, 400 mg oral
ceftibuten once daily has a similar clinical success rate to 500 mg
amoxicillin-
clavulanate three times daily, with a trend toward fewer gastrointestinal side effects, in the treatment of patients with AECB.