Study name |
Fecal microbiota transplantation versus vancomycin or fidaxomicin in Clostridioides difficile infection first recurrence (FENDER) |
Methods |
Open‐label, randomized controlled trial |
Participants |
Inclusion criteria
Adults aged ≥ 18 years at time of informed consent
Informed consent signature
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Medical record documentation of first recurrence of CDI defined as:
previous episode of treated and cured CDI within last 8 weeks confirmed by medical record documentation of a clinical picture of CDI combined with a CDI test performed according to CDI diagnosis ESCMID guidelines
current combination of CDI signs and symptoms, confirmed by medical record documentation of microbiologic evidence of C difficile toxin and C difficile in stools shown by a CDI test performed according to CDI diagnosis ESCMID guidelines, with a mandatory toxin A/B EIA positive test and without reasonable evidence of another cause of diarrhea
No multiple episodes (> 1 recurrence) of CDI that occurred within 3 previous months
Already taking since < 10 days or will start a course of antibiotics (vancomycin or fidaxomicin) to control recurrent CDI symptoms at the time of screening
Willing and able to have FMT by capsule
Exclusion criteria
Complicated CDI (≥ 1 of the following signs or symptoms related to CDI: hypotension requiring vasopressors, ICU admission for a complication of CDI, ileus leading to placement of nasogastric tube, toxic megacolon, colonic perforation, colectomy, or colostomy)
Prior FMT within 6 months of randomization
Prior colectomy, colostomy, ileostomy, or gastrectomy
Metronidazole already given for treatment of first rCDI for > 3 days
Need for continued non‐anti‐CDI systemic antibiotics
Anticipated indication for antibiotics treatment (for a non‐CDI reason) in next 8 weeks
Other infectious causes of diarrhea beyond CDI
Inflammatory bowel disease
Swallowing disorders, Zenker diverticulum, gastroparesis, or prior small bowel obstruction
Known hypersensitivity to vancomycin or fidaxomicin
Pregnant/lactating women
Estimated life expectancy < 10 weeks
Inability to follow protocol study procedures
Inability to give informed consent
Any condition or medications that will put the participant at greater risk from FMT according to the investigator
Severely immunocompromised
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Interventions |
Intervention
Vancomycin 125 mg 4 times daily or fidaxomicin 200 mg 2 times daily, as initially prescribed per standard of care for 10 days, followed 24 hours later by 1 oral FMT (15 capsules administered at day 1 and 15 capsules at day 2), and a second oral FMT depending on recurrent CDI severity
Comparison
Vancomycin 125 mg 4 times daily or fidaxomicin 200 mg 2 times daily, as initially prescribed per standard of care for 10 days
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Outcomes |
Primary outcome
Sustained clinical cure rate. Absence of CDI recurrence (time frame: 8 weeks after study treatment completion)
Secondary outcomes
Treatment failure: early and late CDI recurrence rate (time frame: before 4 weeks and at 5–8 weeks after study treatment completion)
CDI new occurrence rate (time frame: between 8 weeks and 12 months after study treatment completion)
Long‐term clinical cure (time frame: 6 and 12 months after study treatment completion)
Recurrence‐free survival rate from study intervention to CDI recurrence (time frame: 12 months after study treatment completion)
Overall survival from study intervention to death (time frame: 12 months after study treatment completion
Health status EQ‐5D‐5L measure using 5‐digit code (score from 1 to 5 for each digit, 1 representing no problem and 5 representing worse problem) (mobility, self‐care, usual activities, pain/discomfort, anxiety/depression) (time frame: baseline, 8 weeks, 6 and 12 months after study treatment completion)
Health status EQ‐5D‐5L measure using EQ visual analog scale score (0 representing the worst health you can imagine to 100 representing the best health you can imagine) (participant's perception of overall health) (time frame: baseline, 8 weeks, 6 and 12 months after study treatment completion)
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Starting date |
March 2022 |
Contact information |
Benoit Guery MD, Principal Investigator, Centre Hospitalier Universitaire Vaudois, Lausanne, Switzerland |
Notes |
No results posted |