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Obeticholic Acid (OCA) in Primary Sclerosing Cholangitis (PSC) (AESOP)

Primary Purpose

Primary Sclerosing Cholangitis (PSC)

Status

Completed

Phase

Phase 2

Locations

International

Study Type

Interventional

Intervention

Obeticholic Acid (OCA)

Placebo

About this trial

This is an interventional treatment trial for Primary Sclerosing Cholangitis (PSC) focused on measuring PSC

Eligibility Criteria

18 Years - 75 Years (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

Must have had a diagnosis of PSC (based on cholangiography at any point in time).
Alkaline phosphatase at Screening ≥2x ULN.
Total bilirubin at Screening <2.5x ULN.
For participants with concomitant inflammatory bowel disease (IBD):
1. Colonoscopy (if participant has a colon) or other appropriate endoscopic procedure within 12 months of Day 0 confirming no dysplasia or colorectal cancer
2. Participants with Crohn's Disease (CD) must have been in remission as defined by a Crohn's Disease Activity Index (CDAI) <150
3. Participants with ulcerative colitis (UC) must either have been in remission or have had mild disease. Remission was defined as a partial Mayo score of ≤2 with no individual sub-score exceeding 1. Mild disease was defined as a partial Mayo score ≤3 with no individual sub-score exceeding 1 point.
For participants being administered UDCA as part of their standard of care, the dose must have been stable for ≥3 months prior to, and including, Day 0 and must not have exceeded 20 mg/kilograms/day during this time.
Participants being administered biologic treatments (for example, anti-tumor necrosis factor or anti-integrin monoclonal antibodies), immunosuppressants, systemic corticosteroids, or statins, must have been on a stable dose for ≥3 months prior to, and including, Day 0 and should plan to remain on a stable dose throughout the trial.
Contraception: female participants of childbearing potential must have used ≥1 effective method (≤1% failure rate) of contraception during the trial and until 4 weeks following the last dose of IP (including LTSE doses).

Exclusion Criteria:

Evidence of a secondary cause of sclerosing cholangitis at Screening.
Immunoglobulin G4 (IgG4) >4x ULN at Screening or evidence of IgG4 sclerosing cholangitis.
Small duct cholangitis in the absence of large duct disease.
Presence of clinical complications of chronic liver disease or clinically significant hepatic decompensation, including:
- Current Child Pugh classification B or C
- History of, or current diagnosis or suspicion of, cholangiocarcinoma or other hepatobiliary malignancy, or biliary tract dysplasia.
- History of liver transplantation, or current model of end stage liver disease score ≥12
- History of, or current, cirrhosis with complications, including history or presence of spontaneous bacterial peritonitis hepatocellular carcinoma or hepatic encephalopathy (as assessed by the Investigator)
- Current known portal hypertension with complications, including known gastric or large esophageal varices, poorly controlled or diuretic resistant ascites, history of variceal bleeds, or related therapeutic or prophylactic interventions (for example, beta blockers, insertion of variceal bands or transjugular intrahepatic portosystemic shunt).
- History of, or current, hepatorenal syndrome (type I or II) or Screening serum creatinine >2 mg/deciliter (178 micromoles/liter [L]).
- Platelet count <50 x 10^9/L.
Current clinical evidence of dominant strictures that were considered clinically relevant in the opinion of the Investigator or current biliary stent at Screening.
Current cholecystitis or evidence of current biliary obstruction due to gallstones. Asymptomatic gallstones that were not considered a safety risk in the opinion of the Investigator might have been acceptable, subject to discussion and agreement with the Medical Monitor.
Colonic dysplasia within ≤5 years prior to Day 0.
History of small bowel resection.
History of other chronic liver diseases, including, but not limited to, primary biliary cholangitis (PBC), alcoholic liver disease, non-alcoholic fatty liver disease, autoimmune hepatitis, hepatitis B virus (unless seroconverted and no positive Hepatitis B Virus deoxyribonucleic acid), hepatitis C virus and overlap syndrome.
Known Gilbert's syndrome or history of elevations in unconjugated (indirect) bilirubin >ULN or unconjugated (indirect) bilirubin >ULN at Screening.
Known history of human immunodeficiency virus infection.
Currently experiencing, or experienced within ≤3 months of Screening, pruritus requiring systemic or enteral treatment.
Known or suspected acute cholangitis in the 3 months prior to, and including, Day 0 including cholangitis treated with antibiotics.
Administration of antibiotics is prohibited ≤1 month of Day 0 (unless participant was on a stable prophylaxis dose for at least 3 months prior to Day 0).
Administration of the following medications was prohibited ≤6 months of Day 0 and throughout the trial: fenofibrate or other fibrates and potentially hepatotoxic medications (including alpha-methyl-dopa, sodium valproic acid, isoniazide, or nitrofurantoin).
IBD flare during Screening (up to and including Day 0), where "flare" was defined as follows:
- UC flare: partial Mayo Score ≥5, and
- CD flare: CDAI ≥250
Evidence of deleterious effects of alcohol abuse (as assessed by the Investigator) or excessive alcohol consumption (>4 units/day for males, >2 units/day for females).
Known or suspected use of illicit drugs or drugs of abuse (allowed if medically prescribed or indicated) within 3 months of Day 0.
If female: known pregnancy, or had a positive urine pregnancy test (confirmed by a positive serum pregnancy test), or lactating.
Other concomitant disease, malignancy, or condition likely to significantly decrease life expectancy to less than the duration of the trial (for example, moderate to severe congestive heart failure).
Participation in another investigational drug, biologic, or medical device trial within 30 days prior to Screening.
History of noncompliance with medical regimens, or participants who were considered to be potentially unreliable.
Blood or plasma donation within 30 days prior to Day 0.
Mental instability or incompetence such that the validity of informed consent or compliance with the trial was uncertain.

Sites / Locations

St. Joseph's Hospital & Medical Center
Mayo Clinic
University of California Davis Medical Center
University of Colorado, Denver
University of Miami Hospital
Piedmont Atlanta Georgia Transplant Institute
Gastrointestinal Specialists of Georgia
Rush University Medical Center
University of Chicago
Indiana University Health University Hospital
University of Louisville
Tulane Medical Center
Mercy Medical Center
Johns Hopkins University
Henry Ford Health System
Mayo Clinic
Southern Therapy and Advanced Research
St. Louis University Gastroenterology & Hepatology
Washington University School of Medicine
Weill Cornell Medical College
Mount Sinai Medical Center
University of Rochester Medical Center
University Hospitals Cleveland Medical Center
The Ohio State University Wexner Medical Center
University of Pennsylvania
University of Pittsburgh
The Liver Institute at Methodist Dallas Medical Center
Baylor University Medical Center
CHI St. Luke's Health Baylor College of Medicine Medical Center
Liver Associates of Texas, P.A.
Texas Digestive Disease Consultants
McGuire DVAMC
Swedish Organ Transplant and Liver Center
Dipartimento di Universitario di Scienze Mediche e Chirurgiche
Azienda Socio Sanitaria Territoriale di Monza
Azienda Ospedaliera Universita di Padova - Struttura Operativa Complessa Gastroenterologia

Arms of the Study

Arm 1

Arm 2

Arm 3

Arm 4

Arm Type

Experimental

Arm Label

1.5 mg OCA titrating to 3 mg OCA

5 mg OCA titrating to 10 mg OCA

Placebo

LTSE OCA Total

Arm Description

Participants randomized to 1.5 mg OCA took 1.5 mg OCA daily for 12 weeks during the DB phase. If tolerated, the dose was increased to 3 mg OCA daily for an additional 12 weeks.

Participants randomized to 5 mg OCA took 5 mg OCA daily for 12 weeks during the DB phase. If tolerated, the dose was increased to 10 mg OCA daily for an additional 12 weeks.

Participants randomized to placebo took placebo for 24 weeks during the DB phase.

Following completion of the DB phase, participants were asked to reconfirm their consent for participation in the LTSE phase (planned as a further 24 months) beginning at 5 or 10 mg OCA, based on the last treatment received during the DB phase. Doses up to 10 mg daily were evaluated. All participants received open-label OCA during the LTSE phase of the study.

Outcomes

Primary Outcome Measures

DB Phase: Change From Baseline In Serum Alkaline Phosphatase (ALP)

The primary efficacy analysis compared the Week 24 change from Baseline in ALP between OCA treatment group and placebo using an analysis of covariance (ANCOVA) model with fixed effects for treatment group and randomization strata, and Baseline as a covariate. Results are reported in U/L.

LTSE Phase: Incidence Of Adverse Events Of Special Interest (AESIs)

The primary safety analysis evaluated the effects of OCA treatment on AESIs of pruritus, hepatic disorders, and dyslipidemia. All adverse event (AE) summaries were restricted to treatment emergent AEs (TEAEs), which were defined as any AEs that newly appeared, increased in frequency, or worsened in severity following initiation of investigational product. Treatment-emergent pruritus was defined as any preferred term (PT) including "Prur-". Hepatic disorder AESIs were defined using specific Hepatic Disorders Standardized Medical Dictionary for Regulatory Activities (MedDRA) Query (SMQ) terms. AE lipid profile changes, defined in the Dyslipidemia SMQ, were reported. Verbatim terms were mapped to PTs and system organ classes (SOCs) using MedDRA version 17.1 for all AE summaries except those for hepatic disorder AESIs, which used MedDRA version 18.1. A summary of serious and all other non-serious AEs, regardless of causality, is located in the Reported Adverse Events module.

Secondary Outcome Measures

DB Phase: Change From Baseline In Serum Alanine Transaminase (ALT)

As a marker of hepatic biochemistry and liver function, the median change in ALT from Baseline at Week 24 is reported. Results are reported in U/L.

DB Phase: Change From Baseline In Serum Aspartate Aminotransferase (AST)

As a marker of hepatic biochemistry and liver function, the median change in AST from Baseline at Week 24 is reported. Results are reported in U/L.

DB Phase: Change From Baseline In Serum Total Bilirubin

As a marker of hepatic biochemistry and liver function, the median change in serum total bilirubin from Baseline at Week 24 is reported. Results are reported in umol/L.

DB Phase: Change From Baseline In Serum Direct Bilirubin

As a marker of hepatic biochemistry and liver function, the median change in serum direct bilirubin from Baseline at Week 24 is reported. Results are reported in umol/L.

DB Phase: Change From Baseline In Serum Gamma-glutamyl Transferase (GGT)

As a marker of hepatic biochemistry and liver function, the median change in serum GGT from Baseline at Week 24 is reported. Results are reported in U/L.

DB Phase: Change From Baseline In Plasma Fibroblast Growth Factor-19 (FGF-19)

To assess farnesoid X receptor (FXR) activity, the change in FGF-19 from Baseline at Week 24 is reported. Results are reported in picograms/milliliter (pg/mL).

DB Phase: Change From Baseline In Plasma 7α-Hydroxy-4-cholesten-3-one (C4)

To assess FXR activity, the change in plasma C4 from Baseline at Week 24 is reported. Results are reported in nanograms (ng)/mL.

LTSE Phase: Change From Baseline In Serum ALP At Month 12

The median change in serum ALP from Baseline to the last available visit is reported. The DB value at Week 24 was used as the Baseline. Results are reported in U/L.

LTSE Phase: Change From Baseline In Serum ALT At Month 12

As a marker of hepatic biochemistry and liver function, the median change in ALT from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in U/L.

LTSE Phase: Change From Baseline In Serum AST At Month 12

As a marker of hepatic biochemistry and liver function, the median change in AST from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in U/L.

LTSE Phase: Change From Baseline In Serum Total Bilirubin At Month 12

As a marker of hepatic biochemistry and liver function, the median change in serum total bilirubin from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in umol/L.

LTSE Phase: Change From Baseline In Serum Direct Bilirubin At Month 12

As a marker of hepatic biochemistry and liver function, the median change in serum direct bilirubin from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in umol/L.

LTSE Phase: Change From Baseline In Serum GGT At Month 12

As a marker of hepatic biochemistry and liver function, the median change in serum GGT from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in U/L.

LTSE Phase: Change From Baseline In Albumin At Month 12

As a marker of hepatic biochemistry and liver function, the median change in albumin from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in grams (g)/L.

LTSE Phase: Change From Baseline In INR At Month 12

As a marker of hepatic biochemistry and liver function, the median change in INR from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline.

LTSE Phase: Change From Baseline In Transient Elastography (TE) At Month 12

As a marker of hepatic inflammation and fibrosis, the median change in TE, as a measure of hepatic stiffness, from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in kilopascal (kPa).

LTSE Phase: Change From Baseline In Enhanced Liver Fibrosis (ELF) At Month 12

As a marker of hepatic inflammation and fibrosis, the change in ELF score from Baseline at Month 12 is reported. The ELF score and its components (hyaluronic acid [HA]; procollagen-3 N-terminal peptide [P3NP]; tissue inhibitor of metalloproteinase 1 [TIMP-1]) was calculated as follows: 2.278 + 0.851 x ln(HA (ng/mL)) + 0.751 x ln(P3NP (ng/mL)) + 0.394 x ln(TIMP-1 (ng/mL). The DB value at Week 24 was used as the Baseline. An increase in score indicates an improvement/worsening of symptoms.

LTSE Phase: Change From Baseline In Plasma FGF-19 At Month 12

To assess FXR activity, the change in FGF-19 from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in pg/mL.

LTSE Phase: Change From Baseline In Plasma C4 At Month 12

To assess FXR activity, the change in plasma C4 from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in ng/mL.

LTSE Phase: Participants Experiencing Ulcerative Colitis Remission At Month 12

To assess inflammatory bowel disease (IBD) activity, the number of participants experiencing ulcerative colitis remission at Month 12 is reported. Remission was defined as a partial Mayo score of ≤2 with no individual sub-score exceeding 1 point.

LTSE Phase: Participants Experiencing Crohn's Disease Remission At Month 12

To assess IBD activity, the number of participants experiencing Crohn's Disease remission at Month 12 is reported. Remission was defined as a Crohn's Disease Activity Index score of <150.

LTSE Phase: Change From Baseline In Total Bile Acids At Month 12

To assess the effects on bile acids, the median change in total bile acids from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in umol/L.

LTSE Phase: Change From Baseline In Pruritus Visual Analogue Scale (VAS) At Month 12

To assess the effects on disease-specific symptoms, the median change in the pruritus VAS score from Baseline at Month 12 is reported. The score is derived from the VAS participant questionnaire, which has the participant draw a line anywhere on a scale that best represents the severity of the itch; the scale ranges from 0 (no itching) to 10 (worst possible itching), in increments of 2. An increase in score represents an increase in severity of symptoms. The DB value at Week 24 was used as the Baseline.

Full Information

NCT ID

NCT02177136

First Posted

June 26, 2014

Last Updated

June 11, 2021

Sponsor

Intercept Pharmaceuticals

1. Study Identification

Unique Protocol Identification Number

NCT02177136

Brief Title

Obeticholic Acid (OCA) in Primary Sclerosing Cholangitis (PSC)

Acronym

AESOP

Official Title

A Phase 2, Randomized, Double-Blind, Placebo-Controlled, Dose-Finding, Clinical Trial Evaluating the Efficacy and Safety of Obeticholic Acid in Subjects With Primary Sclerosing Cholangitis

Study Type

Interventional

2. Study Status

Record Verification Date

June 2021

Overall Recruitment Status

Completed

Study Start Date

February 9, 2015 (Actual)

Primary Completion Date

March 7, 2017 (Actual)

Study Completion Date

March 22, 2018 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

Intercept Pharmaceuticals

4. Oversight

Studies a U.S. FDA-regulated Drug Product

Yes

Studies a U.S. FDA-regulated Device Product

Data Monitoring Committee

Yes

5. Study Description

Brief Summary

This was a phase 2, double-blind (DB), placebo-controlled trial in participants with primary sclerosing cholangitis to evaluate the effect of obeticholic acid on liver biochemistry, in particular, serum alkaline phosphatase; and, safety. The long-term safety extension (LTSE) phase was conducted to evaluate the safety, tolerability, and efficacy of long-term, open-label use of OCA in participants with PSC who had completed the DB phase of the study.

Detailed Description

This was a phase 2, randomized, double-blind, placebo-controlled, dose-finding evaluation of the efficacy and safety of OCA in participants with PSC. Approximately 75 participants who provided written informed consent and met all of the inclusion and none of the exclusion criteria were randomized to 1 of 3 treatment groups as follows: 1.5 milligrams (mg) titrating to 3 mg OCA, 5 mg titrating to 10 mg OCA, or placebo, in a 1:1:1 ratio. Participants self-administered investigational product (IP) orally, once daily for 2 consecutive 12-week periods. For the first 12 weeks, the participant's dose was 1.5 mg OCA, 5 mg OCA, or placebo. After 12 weeks, the participant's dose was titrated as follows, providing there were no limiting safety or tolerability concerns in the opinion of the Investigator, while maintaining the trial blind: the 1.5 mg OCA treatment group titrated to 3 mg, the 5 mg OCA treatment group titrated to 10 mg OCA, and the placebo group remained on placebo. Double-blind treatment continued for a further 12 weeks at that dose. Any participant whose dose was not titrated, due to safety or tolerability concerns, remained on their starting treatment (1.5 mg OCA, 5 mg OCA, or placebo) for the remainder of the DB phase to Week 24. Randomization was stratified by the presence or absence of concomitant ursodeoxycholic acid (UDCA) use and total bilirubin level (≤1.5x upper limit of normal [ULN] or >1.5x ULN but <2.5x ULN). Following completion of the DB phase, participants were asked to reconfirm their consent for participation in the open-label LTSE phase (planned as a further 24 months).

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study

Primary Sclerosing Cholangitis (PSC)

Keywords

PSC

7. Study Design

Primary Purpose

Treatment

Study Phase

Phase 2

Interventional Study Model

Parallel Assignment

Masking

ParticipantCare ProviderInvestigator

Masking Description

Following completion of the DB phase, participants were asked to reconfirm their consent for participation in the open-label LTSE phase.

Allocation

Randomized

Enrollment

77 (Actual)

8. Arms, Groups, and Interventions

Arm Title

1.5 mg OCA titrating to 3 mg OCA

Arm Type

Experimental

Arm Description

Participants randomized to 1.5 mg OCA took 1.5 mg OCA daily for 12 weeks during the DB phase. If tolerated, the dose was increased to 3 mg OCA daily for an additional 12 weeks.

Arm Title

5 mg OCA titrating to 10 mg OCA

Arm Type

Experimental

Arm Description

Participants randomized to 5 mg OCA took 5 mg OCA daily for 12 weeks during the DB phase. If tolerated, the dose was increased to 10 mg OCA daily for an additional 12 weeks.

Arm Title

Placebo

Arm Type

Experimental

Arm Description

Participants randomized to placebo took placebo for 24 weeks during the DB phase.

Arm Title

LTSE OCA Total

Arm Type

Experimental

Arm Description

Intervention Type

Drug

Intervention Name(s)

Obeticholic Acid (OCA)

Other Intervention Name(s)

6alpha-ethylchenodeoxycholic acid (6-ECDCA), INT-747

Intervention Type

Drug

Intervention Name(s)

Placebo

Primary Outcome Measure Information:

Title

DB Phase: Change From Baseline In Serum Alkaline Phosphatase (ALP)

Description

Time Frame

Baseline, Week 24

Title

LTSE Phase: Incidence Of Adverse Events Of Special Interest (AESIs)

Description

Time Frame

LTSE Baseline (DB Week 24) to Month 26

Secondary Outcome Measure Information:

Title

DB Phase: Change From Baseline In Serum Alanine Transaminase (ALT)

Description

As a marker of hepatic biochemistry and liver function, the median change in ALT from Baseline at Week 24 is reported. Results are reported in U/L.

Time Frame

Baseline, Week 24

Title

DB Phase: Change From Baseline In Serum Aspartate Aminotransferase (AST)

Description

As a marker of hepatic biochemistry and liver function, the median change in AST from Baseline at Week 24 is reported. Results are reported in U/L.

Time Frame

Baseline, Week 24

Title

DB Phase: Change From Baseline In Serum Total Bilirubin

Description

As a marker of hepatic biochemistry and liver function, the median change in serum total bilirubin from Baseline at Week 24 is reported. Results are reported in umol/L.

Time Frame

Baseline, Week 24

Title

DB Phase: Change From Baseline In Serum Direct Bilirubin

Description

As a marker of hepatic biochemistry and liver function, the median change in serum direct bilirubin from Baseline at Week 24 is reported. Results are reported in umol/L.

Time Frame

Baseline, Week 24

Title

DB Phase: Change From Baseline In Serum Gamma-glutamyl Transferase (GGT)

Description

As a marker of hepatic biochemistry and liver function, the median change in serum GGT from Baseline at Week 24 is reported. Results are reported in U/L.

Time Frame

Baseline, Week 24

Title

DB Phase: Change From Baseline In Plasma Fibroblast Growth Factor-19 (FGF-19)

Description

To assess farnesoid X receptor (FXR) activity, the change in FGF-19 from Baseline at Week 24 is reported. Results are reported in picograms/milliliter (pg/mL).

Time Frame

Baseline, Week 24

Title

DB Phase: Change From Baseline In Plasma 7α-Hydroxy-4-cholesten-3-one (C4)

Description

To assess FXR activity, the change in plasma C4 from Baseline at Week 24 is reported. Results are reported in nanograms (ng)/mL.

Time Frame

Baseline, Week 24

Title

LTSE Phase: Change From Baseline In Serum ALP At Month 12

Description

The median change in serum ALP from Baseline to the last available visit is reported. The DB value at Week 24 was used as the Baseline. Results are reported in U/L.

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Serum ALT At Month 12

Description

As a marker of hepatic biochemistry and liver function, the median change in ALT from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in U/L.

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Serum AST At Month 12

Description

As a marker of hepatic biochemistry and liver function, the median change in AST from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in U/L.

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Serum Total Bilirubin At Month 12

Description

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Serum Direct Bilirubin At Month 12

Description

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Serum GGT At Month 12

Description

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Albumin At Month 12

Description

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In INR At Month 12

Description

As a marker of hepatic biochemistry and liver function, the median change in INR from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline.

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Transient Elastography (TE) At Month 12

Description

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Enhanced Liver Fibrosis (ELF) At Month 12

Description

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Plasma FGF-19 At Month 12

Description

To assess FXR activity, the change in FGF-19 from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in pg/mL.

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Change From Baseline In Plasma C4 At Month 12

Description

To assess FXR activity, the change in plasma C4 from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in ng/mL.

Time Frame

LTSE Baseline (DB Week 24), Month 12

Title

LTSE Phase: Participants Experiencing Ulcerative Colitis Remission At Month 12

Description

Time Frame

Month 12

Title

LTSE Phase: Participants Experiencing Crohn's Disease Remission At Month 12

Description

To assess IBD activity, the number of participants experiencing Crohn's Disease remission at Month 12 is reported. Remission was defined as a Crohn's Disease Activity Index score of <150.

Time Frame

Month 12

Title

LTSE Phase: Change From Baseline In Total Bile Acids At Month 12

Description

To assess the effects on bile acids, the median change in total bile acids from Baseline at Month 12 is reported. The DB value at Week 24 was used as the Baseline. Results are reported in umol/L.

Time Frame

Month 12

Title

LTSE Phase: Change From Baseline In Pruritus Visual Analogue Scale (VAS) At Month 12

Description

Time Frame

LTSE Baseline (DB Week 24), Month 12

10. Eligibility

Sex

All

Minimum Age & Unit of Time

18 Years

Maximum Age & Unit of Time

75 Years

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria: Must have had a diagnosis of PSC (based on cholangiography at any point in time). Alkaline phosphatase at Screening ≥2x ULN. Total bilirubin at Screening <2.5x ULN. For participants with concomitant inflammatory bowel disease (IBD): Colonoscopy (if participant has a colon) or other appropriate endoscopic procedure within 12 months of Day 0 confirming no dysplasia or colorectal cancer Participants with Crohn's Disease (CD) must have been in remission as defined by a Crohn's Disease Activity Index (CDAI) <150 Participants with ulcerative colitis (UC) must either have been in remission or have had mild disease. Remission was defined as a partial Mayo score of ≤2 with no individual sub-score exceeding 1. Mild disease was defined as a partial Mayo score ≤3 with no individual sub-score exceeding 1 point. For participants being administered UDCA as part of their standard of care, the dose must have been stable for ≥3 months prior to, and including, Day 0 and must not have exceeded 20 mg/kilograms/day during this time. Participants being administered biologic treatments (for example, anti-tumor necrosis factor or anti-integrin monoclonal antibodies), immunosuppressants, systemic corticosteroids, or statins, must have been on a stable dose for ≥3 months prior to, and including, Day 0 and should plan to remain on a stable dose throughout the trial. Contraception: female participants of childbearing potential must have used ≥1 effective method (≤1% failure rate) of contraception during the trial and until 4 weeks following the last dose of IP (including LTSE doses). Exclusion Criteria: Evidence of a secondary cause of sclerosing cholangitis at Screening. Immunoglobulin G4 (IgG4) >4x ULN at Screening or evidence of IgG4 sclerosing cholangitis. Small duct cholangitis in the absence of large duct disease. Presence of clinical complications of chronic liver disease or clinically significant hepatic decompensation, including: Current Child Pugh classification B or C History of, or current diagnosis or suspicion of, cholangiocarcinoma or other hepatobiliary malignancy, or biliary tract dysplasia. History of liver transplantation, or current model of end stage liver disease score ≥12 History of, or current, cirrhosis with complications, including history or presence of spontaneous bacterial peritonitis hepatocellular carcinoma or hepatic encephalopathy (as assessed by the Investigator) Current known portal hypertension with complications, including known gastric or large esophageal varices, poorly controlled or diuretic resistant ascites, history of variceal bleeds, or related therapeutic or prophylactic interventions (for example, beta blockers, insertion of variceal bands or transjugular intrahepatic portosystemic shunt). History of, or current, hepatorenal syndrome (type I or II) or Screening serum creatinine >2 mg/deciliter (178 micromoles/liter [L]). Platelet count <50 x 10^9/L. Current clinical evidence of dominant strictures that were considered clinically relevant in the opinion of the Investigator or current biliary stent at Screening. Current cholecystitis or evidence of current biliary obstruction due to gallstones. Asymptomatic gallstones that were not considered a safety risk in the opinion of the Investigator might have been acceptable, subject to discussion and agreement with the Medical Monitor. Colonic dysplasia within ≤5 years prior to Day 0. History of small bowel resection. History of other chronic liver diseases, including, but not limited to, primary biliary cholangitis (PBC), alcoholic liver disease, non-alcoholic fatty liver disease, autoimmune hepatitis, hepatitis B virus (unless seroconverted and no positive Hepatitis B Virus deoxyribonucleic acid), hepatitis C virus and overlap syndrome. Known Gilbert's syndrome or history of elevations in unconjugated (indirect) bilirubin >ULN or unconjugated (indirect) bilirubin >ULN at Screening. Known history of human immunodeficiency virus infection. Currently experiencing, or experienced within ≤3 months of Screening, pruritus requiring systemic or enteral treatment. Known or suspected acute cholangitis in the 3 months prior to, and including, Day 0 including cholangitis treated with antibiotics. Administration of antibiotics is prohibited ≤1 month of Day 0 (unless participant was on a stable prophylaxis dose for at least 3 months prior to Day 0). Administration of the following medications was prohibited ≤6 months of Day 0 and throughout the trial: fenofibrate or other fibrates and potentially hepatotoxic medications (including alpha-methyl-dopa, sodium valproic acid, isoniazide, or nitrofurantoin). IBD flare during Screening (up to and including Day 0), where "flare" was defined as follows: UC flare: partial Mayo Score ≥5, and CD flare: CDAI ≥250 Evidence of deleterious effects of alcohol abuse (as assessed by the Investigator) or excessive alcohol consumption (>4 units/day for males, >2 units/day for females). Known or suspected use of illicit drugs or drugs of abuse (allowed if medically prescribed or indicated) within 3 months of Day 0. If female: known pregnancy, or had a positive urine pregnancy test (confirmed by a positive serum pregnancy test), or lactating. Other concomitant disease, malignancy, or condition likely to significantly decrease life expectancy to less than the duration of the trial (for example, moderate to severe congestive heart failure). Participation in another investigational drug, biologic, or medical device trial within 30 days prior to Screening. History of noncompliance with medical regimens, or participants who were considered to be potentially unreliable. Blood or plasma donation within 30 days prior to Day 0. Mental instability or incompetence such that the validity of informed consent or compliance with the trial was uncertain.

Overall Study Officials:

First Name & Middle Initial & Last Name & Degree

George Harb, MD

Organizational Affiliation

Intercept Pharmaceuticals, Inc.

Official's Role

Study Chair

Facility Information:

Facility Name

St. Joseph's Hospital & Medical Center

City

Phoenix

State/Province

Arizona

ZIP/Postal Code

85013

Country

United States

Facility Name

Mayo Clinic

City

Phoenix

State/Province

Arizona

ZIP/Postal Code

85054

Country

United States

Facility Name

University of California Davis Medical Center

City

Sacramento

State/Province

California

ZIP/Postal Code

95817

Country

United States

Facility Name

University of Colorado, Denver

City

Aurora

State/Province

Colorado

ZIP/Postal Code

80045

Country

United States

Facility Name

University of Miami Hospital

City

Miami

State/Province

Florida

ZIP/Postal Code

33136

Country

United States

Facility Name

Piedmont Atlanta Georgia Transplant Institute

City

Atlanta

State/Province

Georgia

ZIP/Postal Code

30309

Country

United States

Facility Name

Gastrointestinal Specialists of Georgia

City

Marietta

State/Province

Georgia

ZIP/Postal Code

30060

Country

United States

Facility Name

Rush University Medical Center

City

Chicago

State/Province

Illinois

ZIP/Postal Code

60612

Country

United States

Facility Name

University of Chicago

City

Chicago

State/Province

Illinois

ZIP/Postal Code

60637

Country

United States

Facility Name

Indiana University Health University Hospital

City

Indianapolis

State/Province

Indiana

ZIP/Postal Code

46202

Country

United States

Facility Name

University of Louisville

City

Louisville

State/Province

Kentucky

ZIP/Postal Code

40202

Country

United States

Facility Name

Tulane Medical Center

City

New Orleans

State/Province

Louisiana

ZIP/Postal Code

70112

Country

United States

Facility Name

Mercy Medical Center

City

Baltimore

State/Province

Maryland

ZIP/Postal Code

21202

Country

United States

Facility Name

Johns Hopkins University

City

Baltimore

State/Province

Maryland

ZIP/Postal Code

21287

Country

United States

Facility Name

Henry Ford Health System

City

Detroit

State/Province

Michigan

ZIP/Postal Code

48202

Country

United States

Facility Name

Mayo Clinic

City

Rochester

State/Province

Minnesota

ZIP/Postal Code

55905

Country

United States

Facility Name

Southern Therapy and Advanced Research

City

Jackson

State/Province

Mississippi

ZIP/Postal Code

39216

Country

United States

Facility Name

St. Louis University Gastroenterology & Hepatology

City

Saint Louis

State/Province

Missouri

ZIP/Postal Code

63104

Country

United States

Facility Name

Washington University School of Medicine

City

Saint Louis

State/Province

Missouri

ZIP/Postal Code

63110

Country

United States

Facility Name

Weill Cornell Medical College

City

New York

State/Province

New York

ZIP/Postal Code

10021

Country

United States

Facility Name

Mount Sinai Medical Center

City

New York

State/Province

New York

ZIP/Postal Code

10029

Country

United States

Facility Name

University of Rochester Medical Center

City

Rochester

State/Province

New York

ZIP/Postal Code

14642

Country

United States

Facility Name

University Hospitals Cleveland Medical Center

City

Cleveland

State/Province

Ohio

ZIP/Postal Code

44106

Country

United States

Facility Name

The Ohio State University Wexner Medical Center

City

Columbus

State/Province

Ohio

ZIP/Postal Code

43210

Country

United States

Facility Name

University of Pennsylvania

City

Philadelphia

State/Province

Pennsylvania

ZIP/Postal Code

19104

Country

United States

Facility Name

University of Pittsburgh

City

Pittsburgh

State/Province

Pennsylvania

ZIP/Postal Code

15213

Country

United States

Facility Name

The Liver Institute at Methodist Dallas Medical Center

City

Dallas

State/Province

Texas

ZIP/Postal Code

75203

Country

United States

Facility Name

Baylor University Medical Center

City

Dallas

State/Province

Texas

ZIP/Postal Code

75246

Country

United States

Facility Name

CHI St. Luke's Health Baylor College of Medicine Medical Center

City

Houston

State/Province

Texas

ZIP/Postal Code

77030

Country

United States

Facility Name

Liver Associates of Texas, P.A.

City

Houston

State/Province

Texas

ZIP/Postal Code

77030

Country

United States

Facility Name

Texas Digestive Disease Consultants

City

Southlake

State/Province

Texas

ZIP/Postal Code

76092

Country

United States

Facility Name

McGuire DVAMC

City

Richmond

State/Province

Virginia

ZIP/Postal Code

23249

Country

United States

Facility Name

Swedish Organ Transplant and Liver Center

City

Seattle

State/Province

Washington

ZIP/Postal Code

98104

Country

United States

Facility Name

Dipartimento di Universitario di Scienze Mediche e Chirurgiche

City

Bologna

ZIP/Postal Code

40138

Country

Italy

Facility Name

Azienda Socio Sanitaria Territoriale di Monza

City

Monza

ZIP/Postal Code

20900

Country

Italy

Facility Name

Azienda Ospedaliera Universita di Padova - Struttura Operativa Complessa Gastroenterologia

City

Padova

ZIP/Postal Code

35128

Country

Italy

12. IPD Sharing Statement

Citations:

PubMed Identifier

32165251

Citation

Kowdley KV, Vuppalanchi R, Levy C, Floreani A, Andreone P, LaRusso NF, Shrestha R, Trotter J, Goldberg D, Rushbrook S, Hirschfield GM, Schiano T, Jin Y, Pencek R, MacConell L, Shapiro D, Bowlus CL; AESOP Study Investigators. A randomized, placebo-controlled, phase II study of obeticholic acid for primary sclerosing cholangitis. J Hepatol. 2020 Jul;73(1):94-101. doi: 10.1016/j.jhep.2020.02.033. Epub 2020 Mar 10.

Results Reference

result

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Obeticholic Acid (OCA) in Primary Sclerosing Cholangitis (PSC)

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