Liver Cirrhosis Clinical Trial
— ZEALOfficial title:
A Two Part Phase IIa/b Multicentre, Randomised, Double-Blind, Placebo-Controlled, Parallel Group Dose-ranging Study to Assess Efficacy, Safety, and Tolerability of the Combination of Zibotentan and Dapagliflozin, and Dapagliflozin Monotherapy Versus Placebo in Participants With Cirrhosis With Features of Portal Hypertension
This is a two part Phase IIa/b multicentre, randomised, double-blind, placebo-controlled, parallel group dose-ranging study to assess the efficacy, safety, and tolerability of the combination of zibotentan and dapagliflozin, and dapagliflozin monotherapy versus placebo in participants with cirrhosis with features of portal hypertension.
| Status | Recruiting |
| Enrollment | 195 |
| Est. completion date | April 16, 2025 |
| Est. primary completion date | January 22, 2025 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 18 Years to 80 Years |
| Eligibility | Study principal inclusion criteria For both Part A and Part B 1. No current or prior (within 1 month of enrolment) medical treatment with an SGLT2 inhibitor or ERAs. 2. On no or a stable dose of beta blockers, with no major dose changes within 1 month prior to the first dose of study intervention. 3. Provision of signed and dated, written ICF prior to any mandatory study-specific procedures, sampling, and analyses. 4. Female participants of non-childbearing potential confirmed at screening by fulfilling one of the following criteria: 1. Post-menopausal: defined as amenorrhoea for at least 12 months or more following cessation of all exogenous hormonal treatments; and also, FSH levels in the post-menopausal range by central laboratory. 2. Documentation of irreversible surgical sterilisation by hysterectomy, bilateral oophorectomy or bilateral salpingectomy but not tubal ligation. 5. Female participants must have a negative pregnancy test at screening and must not be lactating Part A participants who have the following: 1. Clinical and/or histological diagnosis of cirrhosis with either (i) features of portal hypertension or (ii) liver stiffness = 21 kPa. 2. MELD score < 15. 3. Child-Pugh score = 6. 4. No clinically evident ascites. 5. No evidence of worsening of hepatic function (eg, no clinically significant change in signs, symptoms, or laboratory parameters of hepatic disease status) within the last month prior to dosing, as determined by the investigator or usual practitioner. 6. HVPG recording of good enough quality as judged by a central reader. Part B participants who have the following: 1. Clinical and/or histological diagnosis of cirrhosis and either history of decompensation or compensated cirrhosis with signs of clinically significant portal hypertension. 2. HVPG recording of good enough quality and HVPG > 10 mmHg, as judged by a central reader. 3. MELD score < 15. 4. Child-Pugh score < 10. 5. No ascites or ascites up to grade 2 without change in diuretic treatment within the last month prior to first dose and no paracentesis within the last month or planned paracentesis in the next 4 months at screening. 6. No evidence of worsening of hepatic function (eg, no clinically significant change in signs, symptoms, or laboratory parameters of hepatic disease status) within the last month prior to dosing, as determined by the investigator or usual practitioner. Study principal exclusion criteria: 1. Any evidence of a clinically significant disease which in the investigator's opinion makes it undesirable for the participant to participate in the study. 2. Liver cirrhosis caused by chronic cholestatic liver disease 3. ALT or AST = 150 U/L and/or total bilirubin = 3 × ULN 4. Acute liver injury caused by drug toxicity or by an infection. 5. Any history of hepatocellular carcinoma. 6. Liver transplant or expected liver transplantation within 6 months of screening. 7. History of TIPS or a planned TIPS within 6 months from enrolment into the study. 8. Active treatment for HCV within the last 1 year or HBV antiviral therapy for less than 1 year. 9. Participants with T1DM. Medical Conditions (Part A only) 1. INR > 1.5. 2. Serum/plasma levels of albumin = 35 g/L. 3. Platelet count < 75 × 109/L. 4. History of ascites 5. History of hepatic hydrothorax 6. History of portopulmonary syndrome 7. History of hepatic encephalopathy 8. History of variceal haemorrhage 9. History of acute kidney injury 10. History of heart failure, including high output heart failure (eg, due to hyperthyroidism or Paget's disease) Medical Conditions (Part B only) 1. INR > 1.7. 2. Serum/plasma levels of albumin = 28 g/L. 3. Platelet count < 50 × /109L. 4. Acute kidney injury within 3 months of screening. 5. History of encephalopathy of West Haven grade 2 or higher. 6. History of variceal haemorrhage within 6 months prior to screening. 7. NYHA functional heart failure class III or IV or with unstable heart failure requiring hospitalisation for optimisation of heart failure treatment and who are not yet stable on heart failure therapy within 6 months prior to screening. 8. Heart failure due to cardiomyopathies that would primarily require specific other treatment: eg, cardiomyopathy due to pericardial disease, amyloidosis or other infiltrative diseases, cardiomyopathy related to congenital heart disease, primary hypertrophic cardiomyopathy, cardiomyopathy related to toxic or infective conditions (ie, chemotherapy, infective myocarditis, septic cardiomyopathy). 9. High output heart failure (eg, due to hyperthyroidism or Paget's disease). 10. Heart failure due to primary cardiac valvular disease/dysfunction, severe functional mitral or tricuspid valve insufficiency, or planned cardiac valve repair/replacement. |
| Country | Name | City | State |
|---|---|---|---|
| Australia | Research Site | Clayton | |
| Australia | Research Site | Heidelberg | |
| Austria | Research Site | Wien | |
| Belgium | Research Site | Edegem | |
| Canada | Research Site | Edmonton | Alberta |
| China | Research Site | Beijing | |
| China | Research Site | Chengdu | |
| China | Research Site | Chengdu | |
| China | Research Site | Guangzhou | |
| China | Research Site | Hangzhou | |
| Czechia | Research Site | Praha | |
| Czechia | Research Site | Praha | |
| Denmark | Research Site | Aarhus N | |
| Denmark | Research Site | Esbjerg | |
| Denmark | Research Site | Hvidovre | |
| Denmark | Research Site | Køge | |
| France | Research Site | Clichy | |
| France | Research Site | Paris Cedex 13 | |
| France | Research Site | Toulouse | |
| France | Research Site | TOURS Cedex 9 | |
| Germany | Research Site | Dresden | |
| Germany | Research Site | Jena | |
| Germany | Research Site | Landshut | |
| Germany | Research Site | Leipzig | |
| Germany | Research Site | Magdeburg | |
| Germany | Research Site | Mainz | |
| Germany | Research Site | Münster | |
| Germany | Research Site | Wiesbaden | |
| Netherlands | Research Site | Amsterdam | |
| Spain | Research Site | Barcelona | |
| Spain | Research Site | Barcelona | |
| Spain | Research Site | Barcelona | |
| Spain | Research Site | Madrid | |
| Spain | Research Site | Madrid | |
| Spain | Research Site | Majadahonda | |
| Spain | Research Site | Santander | |
| Spain | Research Site | Sevilla | |
| Spain | Research Site | Zaragoza | |
| Switzerland | Research Site | Bern | |
| Switzerland | Research Site | Lugano | |
| Switzerland | Research Site | Luzern | |
| Switzerland | Research Site | St. Gallen | |
| Taiwan | Research Site | Taipei | |
| Taiwan | Research Site | Taipei | |
| United Kingdom | Research Site | Birmingham | |
| United Kingdom | Research Site | Cambridge | |
| United Kingdom | Research Site | London | |
| United Kingdom | Research Site | Nottingham | |
| United States | Research Site | Birmingham | Alabama |
| United States | Research Site | Boston | Massachusetts |
| United States | Research Site | Charleston | South Carolina |
| United States | Research Site | Charlottesville | Virginia |
| United States | Research Site | Dallas | Texas |
| United States | Research Site | Milwaukee | Wisconsin |
| United States | Research Site | New Orleans | Louisiana |
| United States | Research Site | New York | New York |
| United States | Research Site | Pasadena | California |
| United States | Research Site | Richmond | Virginia |
| United States | Research Site | Rochester | Minnesota |
| United States | Research Site | Saint Louis | Missouri |
| United States | Research Site | San Diego | California |
| United States | Research Site | San Francisco | California |
| United States | Research Site | West Hollywood | California |
| Lead Sponsor | Collaborator |
|---|---|
| AstraZeneca |
United States, Australia, Austria, Belgium, Canada, China, Czechia, Denmark, France, Germany, Netherlands, Spain, Switzerland, Taiwan, United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Part A: Absolute change in HVPG from baseline to Week 6. | To evaluate the change from baseline in HVPG on zibotentan and dapagliflozin in combination versus placebo. | at Week 6 | |
| Primary | Part B: Absolute change in HVPG from baseline to Week 6. | To evaluate the change from baseline in HVPG on zibotentan and dapagliflozin in combination and dapagliflozin monotherapy versus placebo. | at Week 6 | |
| Secondary | Part A: Percent change in HVPG from baseline to Week 6. | To evaluate the change from baseline in HVPG on zibotentan and dapagliflozin in combination versus placebo. | at Week 6 | |
| Secondary | Part A: HVPG response, where a responder is defined as HVPG < 10 mmHg or a reduction in HVPG of = 1.5 mmHg from baseline to Week 6. | To evaluate the proportion of participants achieving HVPG < 10 mmHg or a reduction in HVPG of = 1.5 mmHg on zibotentan and dapagliflozin versus placebo. | at Week 6 | |
| Secondary | Part A: Evaluation of change in body weight (kg) over time course of study. Percentage and absolute change from baseline in body weight at Week 6. | To evaluate the effect of zibotentan and dapagliflozin in combination versus placebo on change in body weight. | at Week 6 | |
| Secondary | Part A: Percentage and absolute change in total dosage of loop-diuretic equivalents use from baseline to Week 6. | To evaluate the effect of zibotentan and dapagliflozin in combination versus placebo on total loop-diuretic equivalents use. | at Week 6 | |
| Secondary | Part A: Change in total body water, extracellular water and intracellular water volumes from baseline to Week 6. Change in total body fat mass from baseline to Week 6. | To evaluate the effect of zibotentan and dapagliflozin in combination versus placebo on body water volumes and body fat mass. | at Week 6 | |
| Secondary | Part A: Change in systolic and diastolic blood pressure from baseline to Week 6. | To evaluate the effect of zibotentan and dapagliflozin in combination versus placebo on changes in office-based systolic and diastolic blood pressure. | at Week 6 | |
| Secondary | Part B: Percentage change in HVPG from baseline to Week 6. | To evaluate the change from baseline in HVPG on zibotentan and dapagliflozin in combination and dapagliflozin monotherapy versus placebo. | at Week 6 | |
| Secondary | Part B: HVPG response, where a responder is defined as at least 20% decrease or a reduction to or below 12 mmHg in HVPG from baseline to Week 6. | To evaluate the proportion of participants achieving at least 20% decrease in HVPG or a reduction to or below 12 mmHg in HVPG on zibotentan and dapagliflozin in combination and dapagliflozin monotherapy versus placebo. | at Week 6 | |
| Secondary | Part B: Evaluation of change in body weight (kg) over time course of study. Percentage and absolute change from baseline in body weight at Week 6 and Week 16. | To evaluate the effect of zibotentan and dapagliflozin in combination and dapagliflozin monotherapy versus placebo on change in body weight. | at Week 6 and Week 16 | |
| Secondary | Part B: Absolute change in total dosage of loop-diuretic equivalents use from baseline to Week 6 and Week 16. | To evaluate the effect of zibotentan and dapagliflozin in combination and dapagliflozin monotherapy versus placebo on total loop-diuretic equivalents use. | at Week 6 and Week 16 | |
| Secondary | Part B: Change in total body water, extracellular water and intracellular water volumes from baseline to Week 6 and Week 16. Change in total body fat mass from baseline to Week 6 and Week 16. | To evaluate the effect of zibotentan and dapagliflozin in combination and dapagliflozin monotherapy versus placebo on body water volumes and body fat mass. | at Week 6 and Week 16 | |
| Secondary | Part B: Change in systolic and diastolic blood pressure from baseline to Week 6 and Week 16. | To evaluate the effect of zibotentan and dapagliflozin in combination and dapagliflozin monotherapy versus placebo on changes in office-based systolic and diastolic blood pressure. | at Week 6 and Week 16 |
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