Fecal Transplantation for Primary Clostridium Difficile Infection

Phase 3TerminatedNCT03796650

Oslo University Hospital104 enrolled

Overview

In this randomized controlled trial the investigators want to compare the effect of one-time rectal instillation of fecal microbiota transplantation, compared to a ten-day antibiotic course for the treatment of primary Clostridium difficile infection (CDI). The investigators hypothetsize that the instillation of feces from a healthy donor will be non-inferior to vancomycin in inducing a durable cure.

Up to one third of patients with clostridium difficile infection treated with antibiotics experience recurrent or relapsing symptoms within a few weeks. Even with subsequent antibiotic treatment, multiple recurrences/relapses are frequent. Fecal microbiota transplantation (FMT) has been shown to be significantly more effective in curing recurrent CDI than repeated antibiotic treatment. In current guidelines, FMT is proposed as a treatment option after multiple recurrences/relapses of CDI. The rationale to reserve transplantation of donor feces for recurrent and difficult cases of CDI is a possible risk of pathogen transmittance and the process of finding a donor and screen for communicable disease. The effect of FMT for recurrent CDI, however, suggests that this therapy may be more effective than antibiotics in inducing a durable cure also for primary CDI. If the therapeutic effect of FMT proves to be equal (non-inferior) or more effective than antibiotics, FMT may be the preferable treatment option due to favourable ecological impact compared to antibiotics. In an era with increasing concerns about overuse of antibiotics and emergence of antibiotic resistant bacteria, it is important to investigate therapeutic alternatives that may reduce the need for antibiotics. This trial is a phase III multicentre, randomized controlled, open-label non-inferiority parallel group trial with two arms (FMT and antibiotics), and is a continuation of the phase II trial IMT for Primary Clostridium Difficile Infection (NCT02301000). In the current trial, patients with Clostridium difficile infection and no previous CDI within 12 months prior to inclusion will be randomized 1:1 to FMT or 10 days of guideline-recommended antibiotic therapy (vancomycin 125 mg four times a day). Patients are recruited in Norwegian hospitals. The investigators plan to use frozen microbiota, because supply is easier to organize, compared to fresh fecal samples. Patients in the FMT treatment group will receive one rectal dose of FMT, originating from screened, healthy donors. Patients who are not cured by the first dose is offered a protocol defined additional FMT treatment. In the case of clinical deterioration, appropriate measures will be undertaken according to current guidelines. Patient treatment outcomes are evaluated after 14, 60 and 365 days from inclusion and treatment initiation. An interim analysis is planned after inclusion of the first 94 patients (corresponding to 50% of the planned number of patients).

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Purpose

TREATMENT

Masking

SINGLE

Enrollment

104

Conditions

Clostridium Difficile Infection

Interventions

Fecal microbiota transplantationOTHER

50 g donor feces suspended in saline with added glycerol, administered by a enema kit.

VancomycinDRUG

Peroral vancomycin 125 mg q.i.d. for ten days.

Eligibility

Sex: ALLMin age: 18 Years

Medical Language ↔ Plain English

Inclusion Criteria: * Patients, ≥18 years with primary C. difficile infection, defined by the following three criteria: 1. Diarrhea as defined by the WHO (≥3 loose stools per day), and 2. Positive stool test for toxin producing C. difficile, and 3. No evidence of previous C. difficile infection during 365 days before enrolment. * Written informed consent Exclusion Criteria: * Known presence of other stool pathogens known to cause diarrhea. * Ongoing antibiotic treatment for other infections that cannot be stopped before study treatment administration. * Inflammatory bowel disease or microscopic colitis. * \< 3 months life expectancy. * Serious immunodeficiency, defined as one of the following: * Ongoing or recent chemotherapy and current or expected neutropenia with neutrophil count of \< 500/μL. * Active severe immunocompromising disease. * Inability to comply with protocol requirements. * Need of intensive care. * Known irritable bowel syndrome, diarrheal type. * Pregnancy or nursing. * Known or suspected toxic megacolon or ileus. * Total or subtotal colectomy, ileostomy or colonostomy. * Contraindications for rectal catheter insertion * Known hypersensitivity or other contraindications to vancomycin

Locations (18)

Vestre Viken HF, Bærum Hospital

Sandvika, Gjettum, Norway

Diakonhjemmet Hospital

Oslo, Oslo County, Norway

Ålesund Sjukehus

Ålesund, Norway

Outcomes

Primary Outcomes

Patients with durable cure

Proportion of patients with primary clinical cure at day 14 after treatment start and no recurrent C. difficile infection during 60 days after treatment start, with the assigned treatment alone.

Time frame: 60 days

Secondary Outcomes

Patients with durable cure with additional treatment.

Proportion of patients with primary clinical cure at day 14 after treatment start and no recurrent C. difficile infection during 60 days after treatment start, with or without the need of additional treatment (FMT, metronidazole or vancomycin).

Time frame: 60 days

Treatment adverse events

Proportion of patients with adverse events.

Time frame: 60 and 365 days

Patients with long-time cure

Proportion of patients with primary clinical cure at day 14 after treatment start and no recurrent C. difficile infection during 60 days after treatment start, and without recurrent C. difficile infection within 365 days after treatment start.

Time frame: 365 days

Health-economic evaluation

Health-economic analysis of the two compared treatment modalities

Time frame: 365 days

Data from ClinicalTrials.gov

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