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NCT02160782 Clinical Trial

Safety and Efficacy Study of LUM001 (Maralixibat) With a Drug Withdrawal Period in Participants With Alagille Syndrome (ALGS)

Alagille Syndrome Clinical Trial

ICONIC

Official title:
Long-Term, Open-Label Study With a Double-Blind, Placebo-Controlled, Randomized Drug Withdrawal Period of LUM001 (Maralixibat), an Apical Sodium-Dependent Bile Acid Transporter Inhibitor (ASBTi), in Patients With Alagille Syndrome

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT02160782
Other study ID # LUM001-304
Secondary ID 2013-005373-43
Status Completed
Phase Phase 2
First received
Last updated
Start date October 28, 2014
Est. completion date May 28, 2020

Study information
Verified date June 2021
Source Mirum Pharmaceuticals, Inc.
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a long-term, open-label study with a double-blind, placebo-controlled, randomized drug withdrawal period in children with Alagille Syndrome (ALGS) designed to evaluate the safety and efficacy of LUM001 (Also known as maralixibat or MRX).

Description:

The study is divided into 6 parts: a 6-week open-label, dose escalation period, a 12-week open-label stable dosing period, a 4-week randomized, double-blind, placebo-controlled drug withdrawal period, a 26-week long-term stable dosing period, and an a 52-week optional follow-up treatment period, and a long-term optional follow-up treatment period for eligible participants who choose to stay on treatment with LUM001.

Recruitment information / eligibility
Status Completed
Enrollment 31
Est. completion date May 28, 2020
Est. primary completion date May 28, 2020
Accepts healthy volunteers No
Gender All
Age group 12 Months to 18 Years
Eligibility Inclusion Criteria: - Male or female between the ages of 12 months and 18 years inclusive. - Diagnosis of ALGS. - Evidence of cholestasis (one or more of the following): 1. Total serum bile acid > 3x ULN for age. 2. Conjugated bilirubin > 1 mg/dL. 3. Fat soluble vitamin deficiency otherwise unexplainable. 4. GGT > 3x ULN for age. 5. Intractable pruritus explainable only by liver disease. - Females of childbearing potential must have a negative serum pregnancy test during Screening. - Males and females of child-bearing potential who are sexually active, or are not currently sexually active during the study, but become sexually active during the period of the study and 30 days following the last dose of study drug, must agree and use acceptable contraception during the trial. - Participant is expected to have a consistent caregiver(s) for the duration of the study. - Informed consent and assent (per IRB/IEC) as appropriate. - Access to phone for scheduled calls from study site. - Caregivers (and age-appropriate participants) must be willing and able to use an eDiary device during the study. - Caregivers (and age-appropriate participants) must digitally accept the licensing agreement in the eDiary software. - Caregivers (and age-appropriate participants) must complete at least 10 eDiary reports (morning or evening) during each of two consecutive weeks of the screening period (maximum possible reports = 14 per week). - Average daily score >2 on the Itch Reported Outcome (ItchRO™) questionnaire (maximum possible daily score of 4) for two consecutive weeks in the screening period, prior to dosing. A daily score is the higher of the scores for the morning and evening ItchRO. The average daily score is the sum of all daily scores divided by the number of days the ItchRO was completed. Inclusion Criteria for participants to be eligible for the 52-week optional follow-up treatment period: - Completed the protocol through the Week 48 visit with no safety concerns. Participants who were discontinued due to safety reasons can be rechallenged if blood tests are back to relatively normal values for this patient population and participant does not meet any of the protocol's stopping rules. The decision will be made by the investigator in consultation with the sponsor medical monitor. - Participants who have undergone a surgical disruption of the enterohepatic circulation will not be eligible to enter into the follow up treatment period. - Participants who were discontinued for other reasons will be considered for the 52-week optional follow-up treatment period on an individual basis. The decision will be made by the investigator in consultation with the sponsor medical monitor. Inclusion Criteria for participants with LUM001dosing interruption <7 days, or >=7 days: - The Participant has either: completed the protocol through the Week 48 visit with no major safety concerns OR discontinued due to safety reasons judged unrelated to the study drug, and laboratory results have returned to levels acceptable for this patient population or individual and participant does not meet any of the protocol's stopping rules at the time of entry into the follow-up period. The decision will be made by the investigator in consultation with the sponsor medical monitor. [Participants who were discontinued for other reasons will be considered on an individual basis.] - Females of childbearing potential must have a negative urine or serum pregnancy test (beta- human chorionic gonadotropin [ß-hCG]) at the time of entry into the long-term optional follow-up treatment period. - Males and females of child-bearing potential who are sexually active, or are not currently sexually active during the study, but become sexually active during the period of the study and 30 days following the last dose of study drug, must agree and use acceptable contraception during the trial. - Informed consent and assent (per IRB/EC) as appropriate. - Access to phone for scheduled calls from study site. - Caregivers (and age-appropriate participants) must be willing and able to use an eDiary device during the study. Exclusion Criteria: - Chronic diarrhea requiring ongoing intravenous fluid or nutritional intervention. - Surgical interruption of the enterohepatic circulation. - Previous liver transplant - Decompensated cirrhosis (ALT >15 x ULN, INR >1.5 [unresponsive to vitamin K therapy], albumin <3.0 g/dL, history or presence of clinically significant ascites, variceal hemorrhage, and/or encephalopathy). - History or presence of other concomitant liver disease. - History or presence of any other disease or condition known to interfere with the absorption, distribution, metabolism or excretion of drugs, including bile salt metabolism in the intestine (eg, inflammatory bowel disease). - History or presence of gallstones or kidney stones. - Known diagnosis of human immunodeficiency virus (HIV) infection. - Cancers, except for in situ carcinoma, or cancers treated at least 5 years prior to Screening with no evidence of recurrence. - Recent medical history or current status that suggests that the participant may be unable to complete the study. - Any female who is pregnant or lactating or who is planning to become pregnant during the study period. - Known history of alcohol or substance abuse. - Administration of bile acid or lipid binding resins within 28 days prior to screening and throughout the trial. - Known hypersensitivity to LUM001 or any of its components. - Receipt of investigational drug, biologic, or medical device within 28 days prior to screening, or 5 half-lives of the study agent, whichever is longer. - History of non-adherence to medical regimens, unreliability, mental instability or incompetence that could compromise the validity of informed consent or lead to nonadherence with the study protocol based upon investigator judgment. - Any other conditions or abnormalities which, in the opinion of the investigator or sponsor medical monitor, may compromise the safety of the participant, or interfere with the participant participating in or completing the study. - Participants weighing over 50 kg at screening. Exclusion Criteria for participants with LUM001 dosing interruption >=7 days: - All exclusion criteria mentioned above apply upon entry into the long-term optional follow-up period, with the exception of participants weighing over 50 kg at screening.

Study Design

Related Conditions & MeSH terms

Intervention

Drug:
LUM001 (Maralixibat)
LUM001, also known as Maralixibat (MRX) will be administered orally Once Daily (OD). To be administered Twice Daily (BID) for patients who are eligible.
Placebo
Placebo will be administered orally once daily during randomized withdrawal period

Locations
Country Name City State
Australia The Royal Children's Hospital Melbourne Parkville Victoria
Australia Children's Hospital Westmead Westmead New South Wales
Belgium Cliniques Universitaires Saint-Luc Brussels
France Hopital Femme Mere Enfant De Lyon Bron
France Hopital Kremlin Bicetre Paris
France Hopital Necker-Enfants Malades Paris
Poland The Children's Memorial Health Institute Warsaw
Spain Hospital Universitario La Paz- Hospital Materno Infantil Madrid
United Kingdom Paediatric Liver Center, Kings College Hospital London

Sponsors (1)
Lead Sponsor Collaborator
Mirum Pharmaceuticals, Inc.

Countries where clinical trial is conducted

Australia,  Belgium,  France,  Poland,  Spain,  United Kingdom, 

Outcome
Type Measure Description Time frame Safety issue
Primary Change From Week 18 to Week 22 in Fasting sBA Levels in Participants Who Had a Reduction in sBA =50% From Baseline to Week 12 or Week 18 The primary efficacy endpoint of this study was the mean change from Week 18 to Week 22 (the RWD period) of fasting sBA levels in participants who had a reduction in sBA =50% from baseline to Week 12 or Week 18 (Modified Intent-to-Treat [MITT] Population). Five participants in the MRX group and 10 participants in the placebo group met the prespecified sBA reduction criteria. Week 18 to Week 22
Secondary Change From Baseline to Week 18 in Fasting sBA Levels This secondary efficacy endpoint is the mean change from baseline to Week 18 in fasting sBA levels Baseline to Week 18
Secondary Change From Baseline to Week 18 in Pruritus as Measured by ItchRO (Obs) This secondary efficacy endpoint is the change from baseline to Week 18 in pruritus as measured by ItchRO(Obs) weekly average morning score. ItchRO scores range from 0 to 4; the higher score indicates increasing itch severity (0 = none; 4 = very severe). Baseline to Week 18
Secondary Change From Baseline to Week 18 in Pruritus as Measured by ItchRO (Pt) This secondary efficacy endpoint is the change from baseline to Week 18 in pruritus as measured by ItchRO(Pt) weekly average morning score Baseline to Week 18
Secondary Change From Week 18 to Week 22 in Pruritus as Measured by ItchRO(Obs) This secondary efficacy endpoint is the change from Week 18 to Week 22 in pruritus as measured by ItchRO(Obs) weekly average morning score. ItchRO scores range from 0 to 4; the higher score indicates increasing itch severity (0 = none; 4 = very severe). Week 18 to Week 22
Secondary Change From Week 18 to Week 22 in Pruritus as Measured by ItchRO(Pt) This secondary efficacy endpoint is the change from Week 18 to Week 22 in pruritus as measured by ItchRO(Pt) weekly average morning score. ItchRO scores range from 0 to 4; the higher score indicates increasing itch severity (0 = none; 4 = very severe). Week 18 to Week 22
Secondary Change From Baseline to Week 18 in Alkaline Phosphatase This secondary efficacy endpoint is the mean change from baseline to Week 18 in ALP Baseline to Week 18
Secondary Change From Week 18 to Week 22 in Alkaline Phosphatase This secondary efficacy endpoint is the mean change from Week 18 to Week 22 in ALP Week 18 to Week 22
Secondary Change From Baseline to Week 18 in Alanine Aminotransferase This secondary efficacy endpoint is the mean change from baseline to Week 18 in ALT Baseline to Week 18
Secondary Change From Week 18 to Week 22 in Alanine Aminotransferase This secondary efficacy endpoint is the mean change from Week 18 to Week 22 in alanine aminotransferase (ALT) Week 18 to Week 22
Secondary Change From Baseline to Week 18 in Total Bilirubin This secondary efficacy endpoint is the mean change from baseline to Week 18 in total bilirubin Baseline to Week 18
Secondary Change From Week 18 to Week 22 in Total Bilirubin This secondary efficacy endpoint is the mean change from Week 18 to Week 22 in total bilirubin Week 18 to Week 22
Secondary Change From Baseline to Week 18 in Direct Bilirubin This secondary efficacy endpoint is the mean change from baseline to Week 18 in direct bilirubin Baseline to Week 18
Secondary Change From Week 18 to Week 22 in Direct Bilirubin This secondary efficacy endpoint is the mean change from Week 18 to Week 22 in direct bilirubin Week 18 to Week 22
See also
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Active, not recruiting NCT05035030 - Long-term Safety and Efficacy of Odevixibat in Patients With Alagille Syndrome Phase 3
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Suspended NCT00571272 - Longitudinal Study of Genetic Causes of Intrahepatic Cholestasis (LOGIC)
Completed NCT02057692 - Evaluation of LUM001 in the Reduction of Pruritus in Alagille Syndrome Phase 2
Active, not recruiting NCT02922751 - FibroScan™ in Pediatric Cholestatic Liver Disease (FORCE)
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Completed NCT02131623 - Validation of the Itch Reported Outcome (ItchRO) Diaries in Pediatric Cholestatic Liver Disease
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Completed NCT02047318 - An Extension Study to Evaluate the Long-Term Safety and Durability of Effect of LUM001 in the Treatment of Cholestatic Liver Disease in Subjects With Alagille Syndrome (ALGS) Phase 2
Completed NCT01903460 - Safety and Efficacy Study of LUM001 in the Treatment of Cholestatic Liver Disease in Patients With Alagille Syndrome Phase 2
Completed NCT01515631 - Characterization of Pulmonary Artery Stenoses in Alagille Syndrome - a Medical Record Review
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Approved for marketing NCT04530994 - A Maralixibat Expanded Access Program for Patients With Cholestatic Pruritus Associated With Alagille Syndrome (ALGS)