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Clinical Trial Details — Status: Not yet recruiting

Administrative data

NCT number NCT06427395
Other study ID # SARO.23.002
Secondary ID
Status Not yet recruiting
Phase Phase 3
First received
Last updated
Start date June 15, 2024
Est. completion date July 18, 2027

Study information

Verified date May 2024
Source Zydus Therapeutics Inc.
Contact Farheen Shaikh
Phone 609-730-1900
Email fshaikh@zydustherapeutics.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Open-Label Extension Study of Saroglitazar Magnesium in Participants With Primary Biliary Cholangitis


Description:

A Multicenter, Open-Label, Extension Clinical trial to evaluate Safety and Efficacy of Saroglitazar Magnesium in Participants with Primary Biliary Cholangitis (PBC)


Recruitment information / eligibility

Status Not yet recruiting
Enrollment 150
Est. completion date July 18, 2027
Est. primary completion date April 18, 2027
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: 1. Must provide written informed consent and agree to comply with the trial protocol 2. Participated and completed SARO.21.001, the double-blind treatment phase study Exclusion Criteria: 1. Consumption of 2 standard drinks per day if male and 1 standard drink per day if female for 3 consecutive months (12 consecutive weeks) throughout double-blind phase till screening. 2. Participants with MELD 3.0 score of 15 or greater 3. History or presence of other concomitant liver diseases at screening: 1. Chronic hepatitis B or C virus (HBV, HCV) infection 2. Primary sclerosing cholangitis (PSC) 3. Alcoholic liver disease 4. Autoimmune hepatitis (AIH)-PBC overlap syndrome 5. Hemochromatosis 6. Non-alcoholic steatohepatitis (NASH) on historical biopsy 4. Cirrhosis with complications, including history or presence of: spontaneous bacterial peritonitis, hepatocellular carcinoma, uncontrolled ascites, encephalopathy, history of variceal bleeding or history of hepatorenal syndrome at screening. 5. Use of Thiazolidinediones or Fibrates (within 12 weeks prior to screening) 6. Use of Obeticholic acid (OCA), methotrexate, budesonide and other systemic corticosteroids (Prednisone dose more than 10 mg); potentially hepatotoxic drugs (including a-methyl-dopa, sodium valproic acid, isoniazid, or nitrofurantoin) (within 12 weeks prior to screening) 7. History of bowel surgery (gastrointestinal [bariatric] surgery in the preceding 1 year or undergoing evaluation for gastrointestinal surgery (bariatric surgery for obesity, extensive small-bowel resection) or orthotopic liver transplant (OLT) or listed for OLT 8. Unstable cardiovascular disease, including: 1. Unstable angina, (i.e., new or worsening symptoms of coronary heart disease in the 12 weeks before screening and throughout the screening period), acute coronary syndrome in the 24 weeks before screening and throughout the screening period, acute myocardial infarction in the 12 weeks before screening and throughout the screening period or heart failure of New York Heart Association class (III - IV) or worsening congestive heart failure, or coronary artery intervention, in the 24 weeks before screening and throughout the screening period 2. History/current unstable cardiac dysrhythmias 3. Uncontrolled hypertension at screening 4. Stroke or transient ischemic attack in the 24 weeks before screening 9. History of intracranial hemorrhage, arteriovenous malformation, bleeding disorder, and coagulation disorders 10. An uncontrolled thyroid disorder 1. Uncontrolled hyperthyroidism: defined as any history of hyperthyroidism that has either not been treated with either radioactive iodine and/or surgery or that has been treated with radioactive iodine and/or surgery, but has required ongoing continuous or intermittent use of thyroid hormone synthesis inhibitors (i.e., methimazole or propylthiouracil) in the 24 weeks before screening 2. Uncontrolled hypothyroidism: defined as initiation of thyroid hormone replacement therapy or dose adjustment of replacement therapy in the 12 weeks before screening 11. History of myopathies or evidence of active muscle disease demonstrated by CPK = 5 × ULN at screening 12. Any of the following laboratory values: 1. Total bilirubin > 3 x ULN 2. Platelets < 50 × 103/mL 3. Albumin < 2.8 g/dL 4. eGFR < 45 mL/min/1.73 m2 5. ALT or AST > 250 U/L x ULN 6. ALP > 10 × ULN 13. Participation in another interventional clinical study and receipt of any other investigational medication or medical device within 30 days or within 5 half-lives, whatever is longer, prior to screening 14. History of malignancy in the past 5 years and/or active neoplasm which may diminish life expectancy (except resolved superficial non-melanoma skin cancer, carcinomas in situ or other stable, relatively benign conditions if appropriately treated prior to screening) 15. Known allergy, sensitivity or intolerance to the study medication or formulation ingredients 16. Pregnancy-related exclusions, including: 1. Pregnant/lactating female (including positive pregnancy test at screening) 2. Participants agree to avoid pregnancy either by true abstinence or the use of an acceptable effective contraceptive measures for the duration of the study and for at least 1 month after the end of the study medication. Refer Appendix 9 Contraceptive Guidance. 17. History or other evidence of severe illness or any other conditions that would make the participant, in the opinion of the investigator, unsuitable for the study (such as poorly controlled psychiatric disease, HIV, coronary artery disease or active gastrointestinal conditions that might interfere with drug absorption) 18. Cirrhosis with Child-Pugh-Turcotte (CPT) class B or C having score of 7 or above at screening (Refer Appendix 11

Study Design


Intervention

Drug:
Saroglitazar Magnesium 1 mg
Saroglitazar Magnesium 1 mg will be assigned to all participants enrolled in the open label extension program

Locations

Country Name City State
Argentina Zydus AR001 Ciudad Autónoma de Buenos Aires Buenos Aires
Argentina Zydus AR003 Ciudad Autónoma de Buenos Aires Buenos Aires
Argentina Zydus AR005 Ciudad Autónoma de Buenos Aires Buenos Aires
Argentina Zydus AR006 Ciudad Autónoma de Buenos Aires Buenos Aires
Argentina Zydus AR007 Ciudad Autónoma de Buenos Aires Buenos Aires
Argentina Zydus AR009 Mar del Plata Buenos Aires
Argentina Zydus AR004 Pilar Buenos Aires
Argentina Zydus AR010 Rosario Santa Fe
Turkey Zydus TR014 Adana
Turkey Zydus TR016 Altindag
Turkey Zydus TR004 Ankara
Turkey Zydus TR005 Bursa
Turkey Zydus TR017 Cebeci
Turkey Zydus TR008 Gaziantep
Turkey Zydus TR001 Istanbul
Turkey Zydus TR003 Istanbul
Turkey Zydus TR009 Istanbul
Turkey Zydus TR010 Istanbul
Turkey Zydus TR002 Izmir
Turkey Zydus TR013 Izmir
Turkey Zydus TR011 Kocaeli
Turkey Zydus TR015 Melikgazi
Turkey Zydus TR006 Mersin
United States Zydus US022 Aurora Colorado
United States Zydus US007 Birmingham Alabama
United States Zydus US002 Charlotte North Carolina
United States Zydus US016 Charlottesville Virginia
United States Zydus US014 Cincinnati Ohio
United States Zydus US004 Houston Texas
United States Zydus US042 Houston Texas
United States Zydus US001 Indianapolis Indiana
United States Zydus US027 Jacksonville Florida
United States Zydus US006 Lakewood Ranch Florida
United States Zydus US013 Los Angeles California
United States Zydus US020 Marietta Georgia
United States Zydus US005 Miami Florida
United States Zydus US031 Murray Utah
United States Zydus US037 New Haven Connecticut
United States Zydus US024 Omaha Nebraska
United States Zydus US011 Pasadena California
United States Zydus US015 Philadelphia Pennsylvania
United States Zydus US039 Richmond Virginia
United States Zydus US023 Rochester Minnesota
United States Zydus US035 Rochester New York
United States Zydus US043 Sacramento California
United States Zydus US030 Saint Louis Missouri
United States Zydus US033 Seattle Washington

Sponsors (1)

Lead Sponsor Collaborator
Zydus Therapeutics Inc.

Countries where clinical trial is conducted

United States,  Argentina,  Turkey, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of participants with treatment-related adverse events as assessed by CTCAE v5.0 From baseline to 24 Months/EOT
Secondary Proportion of participants achieving biochemical response based on the composite endpoints of ALP and total bilirubin ALP < 1.67 x ULN, = 15% decrease in ALP, and total bilirubin = ULN or direct bilirubin = ULN relative to baseline in participants with known Gilbert's syndrome From baseline to Months 12 and 24/EOT
Secondary Proportion of participants with biochemical response based on the composite endpoints of ALP and total bilirubin complete normalization of ALP. Change and percent change from baseline in ALP From baseline to Months 12 and 24/EOT
Secondary Time to occurrence of the clinical outcome events in study participants with PBC Defined as new onset or recurrence of any of the following:
Hospitalization for new onset or recurrence of variceal bleed
Hepatic encephalopathy (as defined by a West Haven score =2)
New onset ascites requiring treatment
Refractory ascites (requiring large volume paracentesis)
Spontaneous bacterial peritonitis (confirmed by culture from diagnostic paracentesis)
From baseline to 24 Months/EOT
Secondary Time to occurrence of the clinical outcome events based on Model for End Stage Liver Disease 3.0 score Time from enrolment to the first occurrence of Model for End Stage Liver Disease 3.0 score = 15 and 25% increase from baseline as measured on 2 consecutive occasions performed at least two weeks apart with no competing etiologies identified From baseline to 24 Months/EOT
Secondary Time to first occurrence of Liver transplant or placement on a liver transplant list From baseline to 24 Months/EOT
Secondary Time to the occurrence of Death Death (liver and non-liver related) From baseline to 24 Months/EOT
Secondary Effect on liver enzyme parameters Change from baseline in ALT From baseline to Months 12 and 24/EOT
Secondary Effect on liver enzyme parameters Change from baseline in AST From baseline to Months 12 and 24/EOT
Secondary Effect on liver enzyme parameters Change from baseline in GGT From baseline to Months 12 and 24/EOT
Secondary Effect on liver enzyme parameters Change from baseline in total bilirubin From baseline to Months 12 and 24/EOT
Secondary Effect on lipid parameters Change from baseline in TG From baseline to Months 12 and 24/EOT
Secondary Effect on lipid parameters Change from baseline in LDL-C From baseline to Months 12 and 24/EOT
Secondary Effect on lipid parameters Change from baseline in HDL-C From baseline to Months 12 and 24/EOT
Secondary Effect on lipid parameters Change from baseline in VLDL-C From baseline to Months 12 and 24/EOT
Secondary Effect on lipid parameters Change from baseline in total cholesterol From baseline to Months 12 and 24/EOT
Secondary Effect on lipid parameters Change from baseline in non-HDL-C From baseline to Months 12 and 24/EOT
Secondary Effect on liver enzyme parameters Change from baseline in serum bile acids From baseline to Months 12 and 24/EOT
Secondary Effect on disease-related symptoms Change from baseline in quality of life (Primary Biliary Cholangitis- 40) questionnaire domains Scale as Never, Rarely, Sometimes, Most of the time, and Always From baseline to Months 12 and 24/EOT
Secondary Effect on disease-related symptoms Change from baseline in 5-D itch scale Score ranging from 5 to 25, where higher score represents worst itching From baseline to Months 12 and 24/EOT
Secondary Effect on disease-related symptoms Change from baseline in Worst Itch NRS (numerical rating scale) scores 0-10, where 0 is no itch and 10 is worst itch imaginable From baseline to Months 12 and 24/EOT
Secondary Effect on liver stiffness measurement (LSM) assessed by Liver elastography/FibroScan Change from baseline in LSM assessed by Liver elastography/FibroScan From baseline to Months 12 and 24/EOT
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