Liver Cirrhosis Clinical Trial
— PROMISEOfficial title:
PROMISE Trial: A PROspective Randomised Double-blind Parallel Group Placebo-controlled Multicentre Trial of Faecal MIcrobiota tranSplantation to Improve the Primary outcomE (First Hospitalisation Due to Infection) in Patients With Cirrhosis Over 24 Months
Verified date | May 2024 |
Source | King's College London |
Contact | Sue Cheung |
Phone | 020 7848 0532 |
PROMISE[@]kcl.ac.uk | |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
A feasibility trial called PROFIT has previously shown that FMT administered endoscopically into the jejunum in patients with cirrhosis is safe and feasible and have identified some potential mechanisms of action that warrant further interrogation. The aim of the PROMISE Trial is to evaluate the efficacy and mechanisms of action of encapsulated FMT (versus placebo) to reduce infection and mortality in patients with alcohol-related and metabolic dysfunction-Associated Steatotic Liver (MASLD) cirrhosis.
Status | Recruiting |
Enrollment | 300 |
Est. completion date | April 30, 2027 |
Est. primary completion date | November 30, 2026 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 18 Years and older |
Eligibility | Inclusion Criteria: 1. Aged = 18 years 2. Confirmed Alcohol-related (ALD) or Metabolic dysfunction-Associated Steatotic Liver Disease (MASLD) or MASLD-ALD Overlap cirrhosis based on clinical, radiological and/or histological criteria. 3. MELD score 8-16 28 4. Patients with alcohol-related cirrhosis must have been abstinent for a minimum of 4 weeks prior to randomisation. 5. Patients must be deemed to have the capacity to provide written informed consent to participate. Exclusion Criteria: 1. Severe or life-threatening food allergy (e.g., peanut allergy) 2. Pregnancy or planned pregnancy*. Urine testing will be performed at screening to rule out pregnancy in females. 3. Breast-feeding 4. Patients treated for acute variceal bleeding, infection, overt hepatic encephalopathy, bacterial peritonitis or ACLF within 14 days prior to randomisation. 5. Active alcohol consumption of >20 grams/day [1 unit of alcohol contains 10mLs or 8g of alcohol] 6. Had a previous liver transplant 7. Patients with inflammatory bowel disease. 8. Patients with coeliac disease. 9. Patients with a history of prior gastrointestinal resection or surgery that could change the gut microbiome or result in bacterial overgrowth e.g. gastric bypass 10. Active malignancy including hepatocellular carcinoma 11. Patients with an expected life expectancy <6 months or listed for liver transplantation 12. Infected with HIV, hepatitis B or C [patients who have undetectable hepatitis B or C DNA/RNA can be recruited]. 13. Patients who have received antibiotics or probiotics (excluding food stuffs containing 'live bacteria' such as live yoghurts, kefir, fermented vegetables such as sauerkraut/kombucha or cheese) within 7 days prior to randomisation. Protocol Version 3.0 - 03/11/2023 33 14. Swallowing disorder, oral-motor dyscoordination or likely inability/unwillingness to ingest study medication. 15. Patients who have received another investigational drug or device within 4 months prior to randomisation. 16. Patients, who in the opinion of the PI, have a medical condition, or other relevant psychological, familial, or social factor that may jeopardise their health, compliance, or influence the trial integrity in any way. |
Country | Name | City | State |
---|---|---|---|
United Kingdom | Royal Bournemouth Hospital | Bournemouth | |
United Kingdom | Bristol Royal Infirmary | Bristol | |
United Kingdom | Southmead Hospital | Bristol | |
United Kingdom | Royal Derby Hospital | Derby | |
United Kingdom | Ninewells Hospital | Dundee | |
United Kingdom | Queen Elizabeth Hospital | Gateshead | |
United Kingdom | Queen Elizabeth University Hospital | Glasgow | |
United Kingdom | Hull Royal Infirmary | Hull | |
United Kingdom | St. James University Hospital | Leeds | |
United Kingdom | King's College Hospital NHS Foundation Trust | London | |
United Kingdom | St. George's University Hospital NHS Foundation Trust | London | |
United Kingdom | St. Mary's Hospital | London | |
United Kingdom | Freeman Hospital | Newcastle Upon Tyne | |
United Kingdom | Royal Gwent Hospital | Newport | |
United Kingdom | Queen's Medical Centre | Nottingham | |
United Kingdom | Derriford Hospital | Plymouth |
Lead Sponsor | Collaborator |
---|---|
King's College London | BRITISH LIVER TRUST, Guy's and St Thomas' NHS Foundation Trust, Imperial College London, King's College Hospital NHS Trust, St George's, University of London |
United Kingdom,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Defined infection resulting in hospital admission | To evaluate the efficacy of encapsulated FMT to reduce the susceptibility of infection in patients with cirrhosis measured by the time to first infection resulting in hospitalisation. | From date of randomisation until the date of first hospitlisation, assessed up to Month 24. | |
Secondary | Incidence of decompensating events | All types of decompensating events will be included:
i. hepatic encephalopathy, ii. new-onset ascites, iii. variceal bleeding and iv. spontaneous bacterial peritonitis. |
Screening - End of Visit (Month 24) | |
Secondary | Progression to ACLF (Acute on Chronic Liver Failure) i.e. the development of one or more organ failure | Screening - End of Visit (Month 24) | ||
Secondary | All-cause culture-confirmed infection | Screening - End of Visit (Month 24) | ||
Secondary | Incidence of antibiotic usage | Screening - End of Visit (Month 24) | ||
Secondary | Occurrence of AMR (Anti-Microbial Resistance) | (including skin and nose colonisation with methicillin-resistant Staphylococcus aureus (MRSA), vancomycin-resistant Enterococci (VRE), extended spectrum beta-lactamase producing bacteria (ESBL), fluoroquinolone-resistant gram negative and linezolid-resistant Enterococci (LRE). | Screening - End of Visit (Month 24) | |
Secondary | Hospitalisation rates (liver-related and all-cause) (time to event) including the length of stay (time to discharge among hospitalised participants) and admission to high dependency/intensive care. | Screening - End of Visit (Month 24) | ||
Secondary | Change in liver disease severity scores | Child Pugh Score Score range: Min 5 - Max 15 (The higher score, the more worse outcome) | Screening - End of Visit (Month 24) | |
Secondary | Change in liver disease severity scores | MELD Score (Model for End stage Liver Disease) Score range: Min 6 - Max 40 (The higher score, the more worse outcome) | Screening - End of Visit (Month 24) | |
Secondary | Change in liver disease severity scores | UKELD Score (UK for End stage Liver Disease) Score range: Min 40 - Max 80 (The higher score, the more worse outcome) | Screening - End of Visit (Month 24) | |
Secondary | Change in quality of life (EQ-5D-5L) scores | EQ-5D-5L Score (EuroQol-5 Dimension- 5 Levels) Score range: Min 11111 - Max 55555 (The higher score, the more worse outcome) | Screening - End of Visit (Month 24) | |
Secondary | Change in depression and anxiety scores (using HADS) | HADS Score (Hospital Anxiety Depression Scale) Score range: Min 0 - Max 21 (The higher score, the more worse outcome) Data for anxiety and depression to be cateogorised separately. | Screening - End of Visit (Month 24) | |
Secondary | All-cause mortality and liver-related mortality. | Screening - End of Visit (Month 24) | ||
Secondary | Change in alcohol use disorder-related events in patients enrolled with alcohol-related cirrhosis as assessed by the alcohol-use disorders identification test (AUDIT score) | AUDIT Score (Alcohol Use Disorder Identification Test) Score range: Min 0 - Max 40 (The higher score, the more worse outcome) | Screening - End of Visit (Month 24) | |
Secondary | Change in urinary ethyl glucuronide/ethyl sulphate levels if tested as part of the standard of care. | Screening - End of Visit (Month 24) |
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