Synbiotics and Fecal Microbiota Transplantation to Treat Non-Alcoholic Steatohepatitis
NCT ID: NCT05821010
Last Updated: 2024-08-27
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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RECRUITING
PHASE2
48 participants
INTERVENTIONAL
2023-03-17
2026-08-20
Brief Summary
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1. Can NASH be treated by altering the gut microbiota using LFMT capsules?
2. Can NASH be treated using a syntrophic cocktail of synbiotics and will these strains strengthen the effect of FMT?
3. What are the underlying mechanism by which the aforementioned treatments attenuate NASH?
Participants will be treated with FMT-capsules or placebo, and all participants will receive a cocktail of 3 strains of probiotics and one type of prebiotic.
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Detailed Description
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Secondary objective To investigate the mechanisms of A. soehngenii and pasteurized A. muciniphila combined with B. animalis subsp. lactis and FOS with and without conditioned vegan LFMT capsules in reducing NASH in patients with NASH and NASH-fibrosis.
Study design:
Double-blind randomized placebo-controlled intervention study.
Study population:
Patients between age 18-75 years with biopsy-proven NASH obtained up to 32 weeks before screening based on tandem reading of two expert liver pathologists: SAF Steatosis score ≥1, Activity ≥2, Fibrosis \<4; 50% of participants should at least have NASH fibrosis stage 1, 2 or 3 according to the NASH CRN fibrosis staging system.
Intervention:
Recipient participants From day -3 before the first FMT until completion of the study, all recipient participants will receive an oral daily single dose of 5 g FOS. Subsequently, participants will be randomized to lean donor FMT capsules (donors conditioned with WholeFiber) or placebo (blinded design)1.
At baseline (day 0) and at week 8 (day 56) and week 16 (day 112) participants will ingest 21 LFMT or placebo capsules. The study visits will be 8 weeks apart, although a margin of -3 days to +3 days is implemented to take participants schedule and availability into account. In addition, participants will daily take 2 capsules of LFMT or placebo during the whole study period (24 weeks).
The investigators have previously observed that gut microbiota composition in the recipient is affected up to 8-12 weeks after donor FMT1, so this time window ensures a stable donor gut microbiota composition during the study.
During the 24-week intervention period, all participants will take daily doses of 109 A. soehngenii CH-106 cells (dosage based on previous studies including toxicology study)2,3, 1010 B. animalis subsp. lactis BLC1 (a well-studied strain marketed as a probiotic by Sacco SRL) and 3x1010 pasteurized A. muciniphila ATCC BAA-835T cells (dosage based on EFSA approval and obtained from A-Mansia Biotech).
Percutaneous liver biopsies will be performed as a part of screening when participants are theoretically eligible for participation, unless a liver biopsy has been performed in the previous 36 weeks. A tandem-read by two liver pathologists blinded to any other result will determine if patients will be included in the study. At 24 weeks, another liver biopsy will be performed to examine the effect of the FMT, which will also be reviewed by two liver pathologists (again blinded to any other result). The NASH-CRN classification will be assessed on H\&E slides, for steatosis, inflammation and ballooning, and with a Sirius red-stained slide for evaluation of fibrosis. RNA for RNA-sequencing will be isolated.
Differential gene expression will be assessed over time (baseline and 24 weeks) and by treatment allocation (vegan donor FMT versus placebo).
Feces will be collected at baseline, and after week 2, 8, 10, 16, 18, and 24, in order to investigate the changes in gut microbiome. Also, markers of gut barrier function will be assessed.
Blood will be collected at baseline and at 8, 16 and 24 weeks to investigate common liver enzymes, indicators of glycemic control, lipids, and general and more NASH-specific inflammation parameters.
A multiparametric MRI of liver (MRI-PDFF, MR elastography, corrected T1) and of visceral and subcutaneous fat will be performed at baseline and after 24 weeks to estimate visceral and subcutaneous adipose tissue depot volume, hepatic fat content as well as hepatic fibrosis and inflammation.
Continuous glucose measurements will be performed at home using portable devices, during a consecutive period of 1 week (7 days) in the week before baseline, week 1, 9, 17 and 25.
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
QUADRUPLE
Study Groups
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LFMT-capsules
LFMT-capsules. 3 times bulk, and further continuous administration. This arm is also treated pre- and probiotics.
Lyophilized fecal microbiota transplantation capsules
Oral administration (capsule)
A. soehngenii
Oral administration (capsule)
Pasteurized A. muciniphila
Oral administration (capsule)
B. animalis subsp. lactis
Oral administration (capsule)
Fructo-oligosaccharides
Oral administration (dissolved in water)
Placebo
Placebo-capsules. 3 times bulk, and further continuous administration. This arm is also treated pre- and probiotics.
Placebo capsules
Oral administration (capsule)
A. soehngenii
Oral administration (capsule)
Pasteurized A. muciniphila
Oral administration (capsule)
B. animalis subsp. lactis
Oral administration (capsule)
Fructo-oligosaccharides
Oral administration (dissolved in water)
Interventions
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Lyophilized fecal microbiota transplantation capsules
Oral administration (capsule)
Placebo capsules
Oral administration (capsule)
A. soehngenii
Oral administration (capsule)
Pasteurized A. muciniphila
Oral administration (capsule)
B. animalis subsp. lactis
Oral administration (capsule)
Fructo-oligosaccharides
Oral administration (dissolved in water)
Eligibility Criteria
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Inclusion Criteria
* fluency in Dutch or English
* participants should be able to understand the information and give informed consent
Exclusion Criteria
* liver cirrhosis or hepatocellular carcinoma
* hepatitis B and/or C
* auto-immune hepatitis
* Wilson's disease
* primary sclerosing cholangitis
* primary biliary cholangitis
* alpha-1-antitripsine deficiency and hemochromatosis
* history of liver transplant, current placement on a liver transplant list
* use of pre-, pro- or synbiotics
* use of systemic antibiotics 3 month prior to randomization
* use of tamoxifen, methotrexate or amiodarone
* prior or planned bariatric surgery
* active GLP-1 receptor agonist treated diabetes mellitus
* bleeding disorder
* International normalized ratio (INR) of prothrombin time \>1.4 or platelet count \<100 109/L at screening
* anti-platelet/coagulant therapy use which cannot be temporarily discontinued
* any major cardiovascular event within 6 months prior to screening (e.g. myocardial infarction, cerebrovascular accident)
* prolonged compromised immunity (e.g. recent cytotoxic chemotherapy, HIV-infection with a CD4 count \< 240)
* active or prior history of invasive malignancy (except for curatively treated in situ carcinomas \[e.g., cervix\] or non-melanoma skin cancer) unless a complete remission was achieved
* surgery scheduled for the trial duration period, except for minor surgical procedures, in the opinion of the investigator
* pregnant or nursing women
* any condition which, in the investigator's opinion, might jeopardize participants' safety or compliance with the protocol
* participation in another concomitant clinical trial.
18 Years
75 Years
ALL
No
Sponsors
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Academisch Medisch Centrum - Universiteit van Amsterdam (AMC-UvA)
OTHER
Responsible Party
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Onno Holleboom, MD, PhD
Principal Investigator
Principal Investigators
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A.G. Holleboom, MD, PhD
Role: PRINCIPAL_INVESTIGATOR
Amsterdam UMC
Locations
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Amsterdam UMC
Amsterdam, North Holland, Netherlands
Countries
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Central Contacts
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Facility Contacts
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References
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Augustijn QJJ, Grefhorst A, de Groen P, Wortelboer K, Seegers JFM, Gul IS, Suenaert P, Verheij J, de Vos WM, Herrema H, Nieuwdorp M, Holleboom AG. Randomised double-blind placebo-controlled trial protocol to evaluate the therapeutic efficacy of lyophilised faecal microbiota capsules amended with next-generation beneficial bacteria in individuals with metabolic dysfunction-associated steatohepatitis. BMJ Open. 2025 Jan 9;15(1):e088290. doi: 10.1136/bmjopen-2024-088290.
Other Identifiers
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NL81001.018.22
Identifier Type: -
Identifier Source: org_study_id
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