Integrated Therapies for Alcohol Use in Alcohol-associated Liver Disease (ITAALD) Trial

Samer Gawrieh

Status and phase

Enrolling

Phase 2

Conditions

Alcohol-associated Hepatitis

Treatments

Drug: IL-22

Drug: IL-22 (F-652) Placebo

Drug: Prednisone placebo

Drug: Acamprosate

Behavioral: Motivational Enhancement Therapy (MET)

Behavioral: Usual Care

Behavioral: Motivational Interviewing (MI)

Drug: Prednisone

Study type

Interventional

Funder types

Other

NIH

Identifiers

NCT07060638

ITAALD

U24AA026969 (U.S. NIH Grant/Contract)

Details and patient eligibility

About

This is a multicenter, randomized, double-blinded, placebo-controlled trial focused on the treatment of severe alcohol-associated hepatitis (sAH) and alcohol use disorder (AUD).

The primary purpose of the study is to determine whether subjects receiving sAH therapy in addition to AUD treatments will have better alcohol and liver-related outcomes at 6 months compared to sAH therapy plus usual care for AUD. Patients assigned to the AUD treatment will receive Acamprosate and counseling whereas those assigned to AUD standard care will receive brief advice and referral to a 12-step program.

The secondary purpose of the study is to determine if F-652 is safe and effective in treating sAH when compared to prednisone. Subjects will receive F-652 on days 1 and 7 or prednisone for 28 days. Outcomes will be measured by overall survival at 90 days.

Full description

Objectives:

To determine whether interventions directed to treat AUD integrated with sAH therapies will improve a composite endpoint of alcohol and liver-related events at 6 months compared to usual care for AUD (primary endpoint).
To compare 90-day survival in patients receiving F-652 with those receiving up to 28 days of prednisone using the Day-7 Lille score as a stopping rule (secondary endpoint).
To compare one-year overall survival in patients receiving either IL-22 or prednisone with or without acamprosate (secondary endpoint).

Trial design and conduct

The Investigators will conduct a prospective, multicenter, sequentially randomized trial in 216 patients with sAH using a sequentially randomized design for proof of concept. The trial will assess whether integrated treatment of sAH and AUD reduces alcohol- and liver-related events and mortality.

The trial design resembles a 2X2 factorial study, but the AUD treatment assignment [acamprosate + motivational interviewing (MI) + motivational enhancement therapy (MET)] versus usual care (UC), defined as a brief intervention with advice not to drink alcohol-containing beverages and referral to a 12-step program, is done on Day 7 after the start of the sAH treatment. Only survivors of the first 7 days will be randomized to receive the AUD intervention or UC.

The study will be conducted at six clinical sites in the United States selected by the National Institute of Alcoholic Abuse and Alcoholism (NIAAA) and supported by a Data Coordinating Center at Indiana University (DCC). The DCC will also manage the biorepository.

The study will be conducted according to Good Clinical Practice (GCP) and in compliance with local, state, and federal regulatory requirements. Adverse events during the trial will be identified, recorded, assessed for causality, and reported in accordance with FDA guidance. In addition to general assessment, the investigators will specifically focus on (1) rates and types of infection as well as their severity, (2) potential development of drug-induced liver injury, (3) injection site reactions, and (4) hematological adverse events.

This study will be approved by an appropriately convened single IRB, Advarra, and will be monitored by an NIAAA-appointed Data and Safety Monitoring Board (DSMB). The Investigators will conduct this study under an Investigational New Drug (IND) application from the United States Food and Drug Administration (FDA).

It is anticipated that a centrally located investigational pharmacy at Indiana University will dispense the study medications to all participating sites under close coordination from the DCC. The study will provide the participants with F-652, prednisone, matching placebos, and acamprosate.

Duration of Trial by Phase Treatment phase: up to 6 months Follow-up phase: up to two years

Interventions to be tested F-652 vs. prednisone as treatment for sAH. AUD interventions (acamprosate + MI + MET) versus usual care for AUD treatment.

Group assignment:

The Investigators will sequentially randomize the study participants into four treatment groups.

On day 1, participants will be randomized to receive either F-652 or prednisone at a 1-to-1 ratio. Those randomized to receive F-652 will also receive a prednisone placebo; those randomized to receive prednisone will receive the F-652 placebo. Prednisone or prednisone placebo will be stopped if the Day-7 Lille score is >0.45.

On day 7, survivors will be randomized to receive either the AUD intervention (acamprosate + MI + MET) or usual care at a 1-to-1 ratio.

Block randomization will be used to ensure balanced group sizes in randomization.

So, there will be four treatment combinations:

ARM 1: F-652 on days 1 and 7 and matching placebos for prednisone for 28 days and acamprosate for 6 months. MI will be delivered during the hospitalization; MET sessions will be delivered in the first 3 months.

ARM 2: F-652 on days 1 and 7 and matching placebo for prednisone for 28 days and usual care for AUD.

ARM 3: Prednisone for 28 days and matching placebos for F-652 on days 1 and 7 and acamprosate for 6 months. MI will be delivered during the hospitalization; MET sessions will be delivered in the first 3 months.

ARM 4: Prednisone for 28 days and matching placebo for F-652 on days 1 and 7 and usual care for AUD.

Distribution of study drug and placebo Participants or guardians will be instructed on drug timing and dose of these experimental treatments after discharge from the hospital. Study personnel will ensure participants and guardians are knowledgeable about the frequency and amount before the end of the study visit, and an instructional document will be provided.

Enrollment

216 estimated patients

Sex

All

Ages

18 to 70 years old

Volunteers

No Healthy Volunteers

Inclusion and exclusion criteria

Inclusion Criteria

Age ≥18, <70
MELD 20-35 on day of randomization
Definitive or probable diagnosis as defined by the NIAAA criteria
Onset of jaundice (defined as serum total bilirubin >3 mg/dL) within the prior 8 weeks
Ongoing consumption of > 40 gm (for females) and > 60 gm (for males) alcohol daily for 6 months or more with less than 8 weeks of abstinence before onset of jaundice
AST > 50 IU/L,
AST: ALT > 1.5
ALT and AST values < 400 IU/L
and/or histological evidence of AH*

*In patients with possible AH or AH with confounding factors such as possible ischemic hepatitis, possible DILI, uncertain history of alcohol use (e.g., patient denies excessive alcohol use), and atypical/abnormal laboratory tests (e.g., AST < 50 IU/L or > 400 IU/L, AST/ALT ratio < 1.5), antinuclear antibody > 1:160 or SMA > 1:80, a standard of care liver biopsy may be performed during current hospital admission to confirm AH and exclude competing etiologies.
Females of childbearing (reproductive) potential must have a negative serum or urine pregnancy test at screening.

Exclusion Criteria

Active listing for liver transplantation before screening
MELD score <20 or > 35
Uncontrolled infection (persistent positive blood or other body fluid cultures despite 48 hours of antibiotic therapy)
Progressive hemodynamic compromise requiring intravenous pressors
Pneumonia as evidenced by clinical and radiological examination
Renal failure defined by estimated GFR <35 mL/min.
Clinically active C. diff infection
Evidence of other liver diseases (such as autoimmune hepatitis, primary biliary cholangiopathy, primary sclerosing cholangitis, ischemic, sepsis- or drug-induced liver disease)
History or presence of cancer (including hepatocellular carcinoma) other than non- melanoma skin cancer
Prior exposure to systemic corticosteroid (glucocorticoid) or immunosuppressive therapy for more than 2 days within the previous 30 days
Current use of naltrexone or acamprosate.
Clinically significant pancreatitis- abdominal pain, elevated lipase (> 3 X ULN), and at least edema of pancreas with fat-stranding on CT scan
Active gastrointestinal bleeding defined as hematemesis or melena with a decrease in hemoglobin more than 2 g/dl in 24 hours due to gastrointestinal bleeding, or with a decrease in mean arterial BP to < 65 mmHg
Significant concomitant medical illnesses (such as uncontrolled congestive heart failure or COPD or progressive multi-organ failure) as determined by the study investigator
Uncontrolled mental illness as determined by the study investigator
Uncontrolled HBV, HIV, or HCV infection with persistent viremia. However, subjects with controlled (undetectable viral load) HIV and HBV on viral suppressive therapies will be enrolled and subjects with history of HCV will be enrolled if they have evidence of SVR one year prior to enrollment
Active illicit opiates, cocaine, ketamine, or methamphetamine use in the last 30 days.
Uncontrolled diabetes mellitus with A1c > 9
Pregnancy or breastfeeding
Known allergy or intolerance to therapeutic agents to be tested
Unwillingness to stop alcohol use and to undergo AUD treatment
Unwillingness to either abstain from sexual intercourse, or if sexually active, use a reliable method of birth control during the study and for at least 30 days after the last dose of the study medication. Examples of acceptable birth control methods include double barrier method such as condom and occlusive cap (diaphragm or cervical cap) with spermicidal foam/gel/film/cream/suppository; birth control pills, patches, injections, or implants; intrauterine device (IUD); vasectomy and tubal ligation.
Participant has any condition or circumstance that adversely affects the participant, could cause noncompliance with treatment or visits, may impact the interpretation of clinical data, could cause bias, or may otherwise contraindicate the participant's participation in the study.

Trial design

Primary purpose

Treatment

Allocation

Randomized

Interventional model

Sequential Assignment

Masking

Quadruple Blind

216 participants in 4 patient groups

IL-22 (F-652), Prednisone Placebo, Acamprosate, MI and MET

Active Comparator group

Description:

F-652 on days 1 and 7 and matching placebos for prednisone for 28 days and acamprosate for 6 months. MI will be delivered during the hospitalization; MET sessions will be delivered in the first 3 months

Treatment:

Behavioral: Motivational Interviewing (MI)

Behavioral: Motivational Enhancement Therapy (MET)

Drug: Prednisone placebo

Drug: Acamprosate

Drug: IL-22

IL-22 (F-652), Prednisone Placebo, and usual care

Active Comparator group

Description:

F-652 on days 1 and 7 and matching placebo for prednisone for 28 days and usual care for AUD.

Treatment:

Behavioral: Usual Care

Drug: Prednisone placebo

Drug: IL-22

Prednisone, IL-22 (F-652) Placebo, Acamprosate, MI, and MET

Active Comparator group

Description:

Prednisone for 28 days and matching placebos for F-652 on days 1 and 7 and acamprosate for 6 months. MI will be delivered during the hospitalization; MET sessions will be delivered in the first 3 months

Treatment:

Behavioral: Motivational Interviewing (MI)

Drug: Prednisone

Behavioral: Motivational Enhancement Therapy (MET)

Drug: Acamprosate

Drug: IL-22 (F-652) Placebo

Prednisone, IL-22 (F-652) Placebo, and usual care

Active Comparator group

Description:

Prednisone for 28 days and matching placebo for F-652 on days 1 and 7 and usual care for AUD.

Treatment:

Drug: Prednisone