Microbiota trAnSplant ThERaPy In hEpatiC Encephalopathy (MASTERPIECE)

Phase 2Not Yet RecruitingNCT07528690

VA Office of Research and Development162 enrolled

Overview

The goal of this clinical trial is to find out whether changing the microbes in the bowels of Veterans with cirrhosis and hepatic encephalopathy (a condition that affects the brain as a result of liver problems) using capsules made from microbes from healthy people can prevent future episodes of hepatic encephalopathy.

Wartime injuries as well as metabolic disorders can result in liver injury directly or indirectly through PTSD, metabolic disorders, and/or alcohol misuse. These liver injuries culminate in cirrhosis, which affects 4.9 million patients in the US, \>80,000 of whom are Veterans. Moreover, numerous Veterans with cirrhosis remain undiagnosed, suggesting these numbers are an underestimation. A major complication of cirrhosis, which is exacerbated by alcohol misuse and PTSD, is hepatic encephalopathy (HE), which affects \>50% of Veterans with cirrhosis. Current HE therapies are lactulose (inexpensive but difficult to tolerate) and rifaximin (expensive and second line). However, despite these therapies, a large group of patients have recurrent HE episodes. These recurrences worsen clinical (readmissions, falls, death), psychosocial (cumulative brain injury, poor quality of life, disability, stress on the family), and financial outcomes to the patients, families, and the VHA. Microbiota transplant therapy (MTT) or fecal microbiota transplant (FMT) has the potential to interrupt this cycle. There are Phase 1 and Phase 2a randomized controlled trials (RCTs) published that defined safe and acceptable MTT routes for Veterans with HE. MTT was acceptable to most Veterans who were approached. However, the impact of MTT in preventing HE recurrence in a multi-center context is unclear, especially in those on lactulose only versus those on rifaximin. The central hypothesis is: Microbial transplant therapy delivered through capsules will significantly reduce the rate of HE recurrence regardless of lactulose or rifaximin use compared to placebo in a multi-center double-blind, placebo-controlled, randomized clinical trial of Veterans with cirrhosis. In a 6-month double-blind, multi-center, placebo-controlled, randomized clinical trial in Veterans with cirrhosis and HE on lactulose or rifaximin, these specific aims will be used to test this hypothesis: Aim 1:Determine the rate of HE recurrence in MTT versus placebo-randomized groups: Patients from each site will be randomized 1:1 into receiving MTT or placebo capsules, which will be administered twice a day for 2 weeks. Patients will be followed monthly for 6 months. Recurrence of HE will be defined using standard criteria and will be the primary outcome. Stratification by lactulose use alone or lactulose and rifaximin will be performed. Aim 2: Determine the effect of MTT on all-cause hospitalizations, death, and liver transplant compared to placebo. This analysis will study safety outcomes other than HE between the groups. Aim 3: Determine the impact of MTT on systemic inflammation, microbial community structure and function, and donor engraftment over time compared to placebo. In MTT and placebo groups, stool microbiome will be studied for donor engraftment, microbiome structure (stool metagenomics), and microbiome function (targeted and untargeted metabolomics from stool and blood) to determine impact of MTT on recipients and clinical outcomes. Systemic inflammatory changes and antibiotic resistance microbial genes will be analyzed. Individual donor-recipient matching will be studied to evaluate best combinations. Aim 4: Determine the impact of MTT on cognitive testing, health-related quality of life, and daily function. Cognitive testing, validated PROs, and Veterans' input on FMT and the trial will be analyzed. Based on favorable results of our single-center phase 2A trial, 162 patients (half on lactulose alone and half on rifaximin) across the three sites will be included. Compound MTP-101C, which is a standardized form of MTT targeting delivery into the distal intestine, will be used. Three rationally selected donors with high Lachnospiraceae relative abundance to maximize engraftment and study donor-recipient matching will be selected.

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Purpose

PREVENTION

Masking

QUADRUPLE

Enrollment

162

Conditions

Hepatic Encephalopathy Cirrhosis

Interventions

Microbiota transplant therapy (MTT) capsulesBIOLOGICAL

MTP-101-C is manufactured using cGMP protocols in the Molecular and Cellular Therapeutics (MCT) facility at the University of Minnesota.

Placebo capsuleOTHER

Placebo capsule

Eligibility

Sex: ALLMin age: 21 Years

Medical Language ↔ Plain English

Inclusion Criteria: * 21 years of age * Cirrhosis diagnosed by any of the following in a patient with chronic liver disease * Liver Biopsy * Radiologic evidence of varices, cirrhosis or portal hypertension * Laboratory evidence of platelet count \<110,000 or AST/ALT ratio\>1 * Endoscopic evidence of varices or portal hypertensive gastropathy * Prior overt HE (patient can be on lactulose and/or rifaximin 4 weeks stable dosing) * Able to give written, informed consent \[mini-mental status exam (MMSE)\]\>25 at the time of consenting) * For lactulose only group: Prior HE not on rifaximin Exclusion Criteria: * Disease-related: * MELD3.0 score\>22 * WBC count\<1000 * non-elective hospitalization or overt HE episode within 1 month * on dialysis * known untreated, luminal GI cancer * chronic intrinsic GI diseases (ulcerative colitis, Crohn's disease, microscopic colitis, eosinophilic gastroenteritis or celiac disease) * Safety-related: * Current dysphagia * History of aspiration, intestinal obstruction or non-medication induced gastroparesis * Ongoing absorbable antibiotic use * History of anaphylactic food allergy * Allergy to ingredients in the capsules (glycerol, sodium chloride, hypromellose, gellan gum, titanium dioxide, theobroma oil) * Adverse event attributable to prior FMT (7) ASA Class V * Pregnant or nursing patients * Acute illness or fever on the day of planned FMT * History of spontaneous bacterial peritonitis

Locations (3)

CERC (VISN1, West Haven, CT)

West Haven, Connecticut, United States

VA North Texas Health Care System Dallas VA Medical Center, Dallas, TX

Dallas, Texas, United States

Richmond VA Medical Center, Richmond, VA

Richmond, Virginia, United States

Outcomes

Primary Outcomes

Recurrence of Hepatic Encephalopathy (HE)

HE episodes that requires hospitalization, ER visits, or medication changes prompted under medical supervision.

Time frame: 6 months

Secondary Outcomes

Non-elective Hospitalizations

Cirrhosis-related, relatedness to MTT or all-cause

Time frame: 6 months

Death

Time frame: 6 months

Liver transplant

Time frame: 6 months

Health-related quality of life (HRQOL) assessment: Patient-Reported Outcomes Measurement Information System-29 (PROMIS-29)

PROMIS-29 used 29 items that are scored using T-scores (mean = 50, SD = 10) Maximum 100, minimum 0. Changes in t-scores between and within groups will be studied. High score=better

Time frame: 6 months

Health-related quality of life (HRQOL) assessment: Sickness Impact Profile (SIP)

SIP is a 136-item self-report questionnaire assessing health-related dysfunction, yielding a total score (0-100%) and 12 category scores. Higher scores indicate greater dysfunction (worse health). Items are yes/no, weighted based on severity, and sum into physical and psychosocial dimensions.

Time frame: 6 months

Cognitive testing: Psychometric Hepatic Encephalopathy score (PHES)

Psychometric Hepatic Encephalopathy score is a battery of 5 paper-and-pencil tests (NCT-A, NCT-B, SDT, LTT, DST) used to detect minimal hepatic encephalopathy (MHE), often requiring 15 minutes to complete. It measures cognitive speed, attention, and motor skills, with results adjusted for age and education, typically yielding a sum score -4 indicating impairment. Low score indicates worse performance.

Central Contacts

Jasmohan S Bajaj, MD MS

CONTACT

(804) 675-5802 Jasmohan.Bajaj@va.gov

Brian C Davis, MD

CONTACT

(804) 675-5802 brian.davis5@va.gov

Data from ClinicalTrials.gov

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