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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT06016842
Other study ID # CLIN-60190-454
Secondary ID 2023-505251-43-0
Status Recruiting
Phase Phase 3
First received
Last updated
Start date August 31, 2023
Est. completion date October 18, 2030

Study information

Verified date April 2024
Source Ipsen
Contact Ipsen Clinical Study Enquiries
Phone See e mail
Email clinical.trials@ipsen.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The participants of this study will have confirmed Primary Biliary Cholangitis (PBC). Participants will also have inadequate response or intolerance to ursodeoxycholic acid (UDCA) a drug used to treat PBC. PBC is a disease that progresses slowly. It causes damage to the bile ducts in the liver, leading to a build-up of bile acids which causes further damage. The liver damage in PBC may lead to scarring (cirrhosis). PBC may also be associated with multiple symptoms. Many people with PBC may require liver transplant or may die if the disease progresses and a liver transplant is not done. This study will compare a daily dose of elafibranor (the study drug) to a daily dose of placebo (a dummy treatment). Each participant will be in the study up to about 7 years. The main aim of this study is to determine if elafibranor is better than placebo in preventing clinical outcome events showing disease worsening (including progression of disease leading to liver transplant or death). This study will also study the safety of long-term treatment with elafibranor, as well as the impact on symptoms such as itching and tiredness.


Recruitment information / eligibility

Status Recruiting
Enrollment 450
Est. completion date October 18, 2030
Est. primary completion date October 18, 2030
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria : - Male or female participants must be =18 years of age at the time of signing the informed consent. - Participants with a definite or probable diagnosis of primary biliary cholangitis (PBC) - Participants taking ursodeoxycholic acid (UDCA) for at least 12 months (at a stable dose for =3 months) prior to screening period and expected to remain on stable dose during the study, or unable to tolerate UDCA treatment (no UDCA for =3 months) prior to screening period (per country standard-of-care dosing). - Participants taking medications for management of pruritus (e.g. cholestyramine, rifampin, naltrexone, sertraline or colchicine) must be on a stable dose for =3 months prior to screening period. - Contraceptive use by men or women should be consistent with local regulations regarding the methods of contraception for those participating in clinical studies. - Capable of giving signed informed consent which includes compliance with the requirements and restrictions listed in the informed consent form (ICF) and in this protocol. Exclusion Criteria : - History or presence of other concomitant liver disease including but not limited to: i) Primary sclerosing cholangitis (PSC). ii) Autoimmune hepatitis (AIH) by simplified Diagnostic Criteria of the International Autoimmune Hepatitis Group (IAIHG) =6, or if treated for an overlap of PBC with AIH, or if there is clinical suspicion and evidence of overlap AIH features, that cannot be explained alone by insufficient response to UDCA. iii) Positive hepatitis B surface antigen (HBsAg). Participants with negative HBsAg and positive hepatitis B core antibody (HBcAb) may be eligible if hepatitis B virus deoxyribonucleic acid (HBV DNA) is negative. iv) Hepatitis C virus (HCV) infection defined by positive anti-HCV antibody and positive HCV ribonucleic acid (RNA) (Note: Participants with positive anti-HCV antibody due to previously treated HCV infection, may be enrolled if a confirmatory HCV RNA is undetectable and sustained viral response has been documented). v) Alcohol-associated liver disease (ALD). vi) Nonalcoholic steatohepatitis (NASH). vii) Other chronic liver diseases, such as alpha-1 antitrypsin deficiency. - History or presence of clinically significant hepatic decompensation, including: i) History of liver transplantation, current placement on a liver transplant list, current model for end-stage liver disease including serum sodium (MELD)-Na score =12 due to hepatic impairment (MELD-Na will be calculated only when MELD >11). ii) Evidence of complications of cirrhosis, including hepatic decompensation or evidence of significant portal hypertension complications including presence of uncontrolled ascites; history of variceal bleeding or related interventions (e.g. variceal banding, or transjugular intrahepatic portosystemic shunt placement); presence of hepatic encephalopathy Grade 2 or higher per West-Haven criteria; history or presence of spontaneous bacterial peritonitis. Note: participants with low-risk varices (Grade I) without history of bleeding or other treatment may be eligible to enrol. iii) Hepatorenal syndrome (HRS) (type I or II). - Known history of human immunodeficiency virus (HIV) infection or having a positive confirmatory test for HIV type 1 or 2. - Medical conditions that may cause non-hepatic increases in ALP (e.g. Paget's disease). - Evidence of any other unstable or untreated clinically significant immunological, endocrine, hematologic, gastrointestinal, neurological, or psychiatric disease as evaluated by the investigator; other clinically significant conditions that are not well controlled. - Non-hepatic medical conditions that may diminish life expectancy to <2 years, including known cancers. - History of hepatocellular carcinoma. - Alpha-fetoprotein (AFP) >20 ng/mL with 4-phase liver computerised tomography (CT) or magnetic resonance imaging (MRI) imaging suggesting presence of hepatocellular carcinoma. - Known malignancy or history of malignancy within the last 5 years, with the exception of local, successfully treated basal cell carcinoma or in-situ carcinoma of the uterine cervix. - Administration of the following medications is prohibited during the study, and prior to the study as per the timelines specified below: i) 3 months prior to screening period: fibrates, seladelpar, glitazones, obeticholic acid, azathioprine, cyclosporine, methotrexate, mycophenolate, pentoxifylline, budesonide and other systemic corticosteroids (parenteral and oral chronic administration only); potentially hepatotoxic drugs (including a-methyl-dopa, sodium valproic acid, isoniazid or nitrofurantoin). - Participants with previous exposure to elafibranor. - Participants who are currently participating in, plan to participate in, or have participated in an investigational drug study or medical device study containing active substance within 30 days or 5 half-lives, whichever is longer, prior to the screening period. i) If the previous study was for an experimental therapy being studied for potential benefit in PBC, and the potential therapeutic agent was proven to have no beneficial effect in PBC and there are no safety concerns, the participant may enrol after 30 days or 5 half-lives from the last dose of the therapeutic agent, whichever is longer. ii) For therapeutic agents being studied for potential benefit in PBC for which it is still unclear if there may be a potential benefit, participants may enrol after 6 months from the last dose of the therapeutic agent. - Electrocardiogram (ECG) with QT interval corrected by Fridericia's formula (QTcF) >450 msec in males or QTcF >470 msec in females for participants without bundle branch block. For participants with bundle branch block or other intraventricular conduction delay, a longer QTcF >480 msec would be exclusionary. - Total bilirubin (TB) >3x ULN. Participants with Gilbert's syndrome are eligible with a total bilirubin above 3× ULN if direct bilirubin is <30% of total bilirubin. - Alanine aminotransferase (ALT) and/or aspartate aminotransferase (AST) >5x ULN at SV1, or variability >40% based on two consecutive values. The interval between the two measurements should be of at least 2 weeks (and up to 4 weeks): - Creatinine phosphokinase (CPK) >2x ULN. - Platelet count <75,000/µL - International normalised ratio (INR) >1.5 in the absence of anticoagulant therapy. - Estimated glomerular filtration rate (eGFR) <45 mL/min/1.73m2 per the Modification of Diet in Renal Disease (MDRD)-6 Study formula at SV1. - Significant renal disease, including nephritic syndrome, chronic kidney disease (CKD) (defined as participants with evidence of significantly impaired kidney function or underlying kidney injury). - For female participants: known current pregnancy, or has a positive serum pregnancy test, or is breastfeeding. - Regular alcohol intake in excess of the recommended limit of 1 standard drink per day for men or women. - History of alcohol abuse, or other substance abuse within 1 year prior to SV1. - A positive drug screen at screening would be exclusionary unless it can be explained by a prescribed medication. Use of cannabidiol (CBD) or other cannabinoids is not exclusionary for this study. - Known hypersensitivity to elafibranor or to any of the excipients of the investigational product(s). - Mental instability or incompetence, such that the validity of informed consent or ability to be compliant with the study is uncertain. - Any other condition that, in the opinion of the investigator, would interfere with study participation or completion, or would put the participant at risk, including a potential participant assessed as being at high risk of noncompliance with the study.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Elafibranor
Duration: up to an estimated 84-month (7-year) double-blind treatment period during which elafibranor 80 mg tablet will be administered once daily
Other:
Matched 80 mg placebo
Duration: up to an estimated 84-month (7-year) double-blind treatment period during which matching placebo tablet will be administered once daily

Locations

Country Name City State
Czechia Hepato-Gastroenterologie HK, s.r.o. Hradec Králové
Czechia Artroscan Ostrava
France Centre Hospitalier Regional Universitaire de Lille - Hopital Claude Huriez Lille
France Hospices Civils de Lyon (HCL) - Hopital de la Croix-Rousse Lyon
France CHU de Nice, Hopital de l'Archet Nice
France CHU Poitiers Poitiers
Italy Azienda Ospedaliero Universitaria Federico II di Napoli Naples
Italy Azienda Ospedaliera Universitaria Policlinico Paolo Giaccone Palermo
Korea, Republic of Keimyung University Dongsan Hospital Daegu
Korea, Republic of Chung-Ang University Hospital Seoul
Korea, Republic of Hallym University Kangnam Sacred Heart Hospital Seoul
Poland NZOZ Twoje Zdrowie EL Sp. z o.o. Elblag
Poland Krakowskie Centrum Medyczne Sp.z.o.o - FutureMeds Kraków
Poland FutureMeds Warszawa Centrum Warszawa
Romania Centrul Pentru Studiul Metabolismului Bucharest
Romania Sana S.R.L Bucharest
Romania Gastromedica Srl Iasi
Spain Hospital Universitario Vall d'Hebron Barcelona
Spain Clinica Universidad Navarra-Sede Madrid Madrid
Spain Hospital Universitario Virgen de la Victoria Málaga
Spain Hospital Universitario y Politecnico La Fe Valencia
Spain American Research Corporation Valladolid
United States University of Michigan Health System Ann Arbor Michigan
United States Texas Clinical Research Institute Arlington Texas
United States American Research Corporation Austin Texas
United States Peak Gastroenterology Associates Colorado Springs Colorado
United States Gastroenterology Center of the Midsouth Cordova Tennessee
United States Southern California Research Center Coronado California
United States Liver Center of Texas Dallas Texas
United States South Denver Gastroenterology, P.C. Englewood Colorado
United States Liver Associates of Texas Houston Texas
United States Gastro health & Nutrition Katy Texas
United States Arkansas Diagnostic Center, PA Little Rock Arkansas
United States GastroIntestinal BioSciences Los Angeles California
United States American Research Corporation at The Texas Liver Institute San Antonio Texas
United States Louisiana Research Center, LLC Shreveport Louisiana
United States Arizona Liver Health Tucson Arizona
United States Impact Research Tx Waco Texas
United States Liver Institute Northwest Washington Texas

Sponsors (1)

Lead Sponsor Collaborator
Ipsen

Countries where clinical trial is conducted

United States,  Czechia,  France,  Italy,  Korea, Republic of,  Poland,  Romania,  Spain, 

Outcome

Type Measure Description Time frame Safety issue
Primary Event-free survival Event-free survival is defined as the time from start of treatment to either adjucated disease progression or death, whichever occurs first. From baseline until 4 weeks after the end of treatment (maximum duration of 7 years)
Secondary Percentage of participants experiencing Treatment Emergent Adverse Events (TEAEs), treatment-related TEAEs, Serious Adverse Events (SAEs), and Adverse Events of Special Interests (AESIs) An Adverse event (AE) is any untoward medical occurrence, temporally associated with the use of study intervention, whether or not related to the study intervention. AESIs are AEs that may not be serious but are of special importance to a particular drug or class of drugs. From baseline until 4 weeks after the end of treatment (maximum duration of 7 years)
Secondary Percentage of participants developing clinically significant changes in physical examination findings Complete physical examination at screening and targeted examination at all other clinical visit timepoints. From baseline until 4 weeks after the end of treatment (maximum duration of 7 years)
Secondary Percentage of participants developing clinically significant changes in vital signs Percentage of participants with clinically significant changes in Vital Signs will be reported. The clinical significance will be graded by the investigator. From baseline until 4 weeks after the end of treatment (maximum duration of 7 years)
Secondary Percentage of participants developing clinically significant changes in Electrocardiogram (ECG) readings. Percentage of participants with clinically significant changes in ECG readings will be reported. The clinical significance will be graded by the investigator. From baseline until 4 weeks after the end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with clinically significant changes in laboratory parameters (blood chemistry, hematology, coagulation and urinalysis) Percentage of participants with clinically significant change in laboratory parameters (blood chemistry, hematology and coagulation) will be reported. The clinical significance will be graded by the investigator. From baseline until 4 weeks after the end of treatment (maximum duration of 7 years)
Secondary Change from baseline in Alkaline phosphatase (ALP) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in Total Bilirubin (TB) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with ALP= 1.67x ULN and TB= ULN At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with complete biochemical response Defined as normal levels of TB, ALP, transaminases, albumin, and International normalised ratio (INR) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with normalisation of TB and ALP Defined as TB< Upper Limit Normal (ULN) and ALP< ULN At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with stabilisation in TB (i.e. no increase) Defined as TB< 1x ULN or increase from baseline <0.1x ULN At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with a response based on albumin normalisation At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in liver stiffness measurement (LSM) Assessed by vibration-controlled transient elastography (VCTE) using Fibroscan® on the day of the visit. At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in PBC risk scores based in Global PBC Study Group (GLOBE) score The GLOBE score is a validated risk assessment tool providing an estimate of transplant-free survival for patients with PBC. It was developed by the Global PBC Study Group using Cox regression model on over 4,000 patients with PBC. Lower GLOBE score predicts lower risk. It is calculated from the following equation:
GLOBE score = (0.044378 * age + 0.93982 * LN(total bilirubin/ULN) +(0.335648 * LN(alkaline phosphatase/ULN)) - 2.266708 * albumin /LLN -0.002581 * platelet count per 109/L) + 1.216865
GLOBE scoring system, which calculation is based on serum values of bilirubin, ALP, albumin and platelet count after 1 year of treatment and age at baseline. A high number is indicative of a worse score.
At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in PBC risk scores based on United Kingdom (UK)-PBC score. PBC risk score developed by United Kingdom (UK)-PBC Consortium is a scoring system and the calculation is based on laboratory test measurements and upper limits of normal (ULN) for the total bilirubin (BIL12); alanine transaminase or aspartate transaminase (TA12), and alkaline phosphatase (ALP12) after at least 12 months of UDCA, and the laboratory test measurements and lower limits of normal (LLN) for the serum albumin and platelet count in the same timeframe. A high number is indicative of a worse score. At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with LSM =15 kPa Assessed by VCTE using Fibroscan® At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change in serum levels of Aspartate aminotransferase (AST) compared to the baseline At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change in serum levels of ALT compared to the baseline At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change in serum levels of Gamma-glutamyl transferase (GGT) compared to the baseline At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in hepatic function: Conjugated bilirubin At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change in serum levels of Albumin compared to the baseline At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in hepatic function: international normalised ratio (INR) At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in hepatic function: fractionated ALP At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with no worsening of LSM Assessed by VCTE using Fibroscan® defined as no increase >2kPa from baseline At Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with ALP reduction of 40% At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with ALP <1.5x ULN, ALP decrease =15% and TB =ULN At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with ALP <1.5x ULN, ALP decrease =40% and TB =ULN At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with ALP <1.67x ULN, ALP decrease =15% and TB =ULN At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with ALP <3x ULN, AST <2x ULN and TB =1 mg/dL (Paris I) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with ALP =1.5x ULN, AST =1.5x ULN and TB =1 mg/dL (Paris II criteria) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with normalisation of abnormal TB Assessed at Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with normalisation of abnormal TB and albumin (Rotterdam criteria) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with reduction in TB to =0.6x ULN in participants with TB >0.6x ULN at baseline At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in lipid parameters: total cholesterol (TC) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in lipid parameters: high density lipoprotein cholesterol (HDL-C) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in lipid parameters: calculated very low density lipoprotein cholesterol (VLDL-C) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in lipid parameters: low density lipoprotein cholesterol (LDL-C) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in lipid parameters: triglycerides (TG) At Month 6, Month 12, and every 12 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with a response in PBC Worst Itch NRS score Defined as =2-point reduction from baseline NRS in participants with a baseline NRS =4 Through 6 months up to end of treatment (maximum duration of 7 years)
Secondary Percentage of participants with a response in PBC Worst Itch NRS Defined as =3-point reduction from baseline NRS in participants with a baseline NRS =4 Assessed through 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in 5D-Itch scale Questionnaire that assesses symptoms in terms of 5 domains: degree, duration, direction, disability and distribution. Participants rate their symptoms over the preceding 2-week period on a 1 to 5 scale, with 5 being the most affected. Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in Patient Global Impression of Severity (PGI-S) A 1-item, 5-point scale designed to assess the participant's impression of disease severity Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in Patient Global Impression of Change (PGI-C) A 1-item, 5-point scale designed to assess the participant's impression of change in disease severity since the baseline visit Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in Patient Reported Outcome Measurement Information System (PROMIS) Fatigue Short Form 7a Consists of 7 items that measure both the experience of fatigue and the interference of fatigue on daily activities over the past week. Response options are on a 5-point Likert scale, ranging from 1 to 5. Scores can range from 7 to 35, with higher scores indicating greater fatigue. Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in the Epworth Sleepiness Scale (ESS) Self-administered questionnaire that consists of 8 questions asking to rate how likely it is to fall asleep in different situations commonly encountered in daily life (each question can be scored from 0 to 3 points; '0' indicates no sleepiness, '3' indicates significant sleepiness). It provides a total score which has been shown to relate to the participant's level of daytime sleepiness (total score range 0-24 points). Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in PBC-40 score 40-item questionnaire that assesses symptoms across 6 domains: fatigue, emotional and social, cognitive function, general symptoms and itch. Participants respond on a verbal response scale, depending on the section options range from 'never' / 'not at all' / 'strongly disagree' to 'always' / 'very much' / 'strongly agree'. Six items (3/3 in the itch domain, 2/10 in the social domain, and 1/7 in the general symptoms domain) also include a 'does not apply' option. A score for each domain is provided (but a total score is not calculated), with each verbal response scale correlating to a score of 1 to 5 per item (0 to 5 on items with a 'does not apply' option) with 5 being the most affected (greatest burden). The PBC-40 has a 4-week recall period. Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in PBC Worst Itch Numeric Rating Scale (NRS) score Self-administered patient-reported outcome questionnaire that measures itch intensity. It asks participants to rate the intensity of their Worst Itch on an 11-point scale ranging from 0 (no itch) to 10 (Worst Itch imaginable): - once daily (24-hour recall period) using the eDiary during the screening and initial 2 years of the study, - at the clinic visits (7-day recall period), from Year 3 onwards Assessed through 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in EuroQol 5-dimensional 5-level questionnaire (EQ-5D-5L) Self-administered standardised questionnaire that assesses the 5-dimensions of mobility, self-care, usual activities, pain/discomfort, anxiety/depression descriptively (each dimension has 5 levels) and the overall health state via an EQ Visual Analogue Scale (VAS). Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Change from baseline in Work Productivity and Activity Impairment General Health (WPAI-GH) Questionnaire that measures absenteeism, presenteeism as well as the impairments in unpaid activity because of health problem during the past seven days. It consists of 6 questions: 1=currently employed; 2=hours missed because of health problems; 3=hours missed because of other reasons; 4=hours actually worked; 5=degree health affected productivity while working (using a 0 to 10 Visual Analogue Scale (VAS)); 6=degree health affected productivity in regular unpaid activities (VAS). Assessed at every 6 months up to end of treatment (maximum duration of 7 years)
Secondary Time to the first occurrence of each of individual adjudicated clinical outcome events Among: • All-cause mortality • Liver-related mortality • Liver transplantation • Progression to cirrhosis • Progression to clinically significant portal hypertension • MELD-Na score =15 in participants with baseline MELD or MELD-Na score <12 • Liver decompensation • Occurrence of hepatocellular carcinoma From baseline until 4 weeks after the end of treatment
Secondary Area under the plasma concentration-time curve from time 0 to 24 hours: AUC0-24 At Day 1/Baseline, Month 6 and Month 12 (during a dosing period of 24 hours)
Secondary Maximum (peak) plasma drug concentration: Cmax At Day 1/Baseline, Month 6 and Month 12 (during a dosing period of 24 hours)
Secondary Time to reach maximum (peak) plasma concentration following drug administration): Tmax At Day 1/Baseline, Month 6 and Month 12 (during a dosing period of 24 hours)
Secondary Apparent clearance of drug from plasma (CL) At Day 1/Baseline, Month 6 and Month 12 (during a dosing period of 24 hours)
Secondary Apparent volume of distribution (VZ) At Day 1/Baseline, Month 6 and Month 12 (during a dosing period of 24 hours)
See also
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Not yet recruiting NCT03521297 - Probiotics in PBC Patients of Poor Response to UDCA Phase 2
Recruiting NCT05896124 - CS0159 in Chinese Patients With PBC (Primary Biliary Cholangitis) Phase 2
Completed NCT04047160 - Safety, Tolerability of OP-724 in Patients With Primary Biliary Cholangitis (Phase I) Phase 1
Completed NCT03124108 - Study to Evaluate the Efficacy and Safety of Elafibranor in Patients With Primary Biliary Cholangitis (PBC) and Inadequate Response to Ursodeoxycholic Acid Phase 2