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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT05187715
Other study ID # ILBS-Cirrhosis-46
Secondary ID
Status Recruiting
Phase N/A
First received
Last updated
Start date February 26, 2022
Est. completion date October 2023

Study information

Verified date October 2021
Source Institute of Liver and Biliary Sciences, India
Contact Dr Akhil Deshmukh, MD
Phone 01146300000
Email akhildeshmukh52@gmail.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

Hepatopulmonary syndrome (HPS) is a frequent pulmonary complication of end-stage liver disease that is characterized by decreased arterial oxygenation caused by intrapulmonary vascular dilatation. Due to the different diagnostic criteria used in different studies, its prevalence ranges from 4% to 47% in patients with cirrhosis. Main underlaying pathogensis for HPS being activation of macrophages which are responsible for iNOS, PDGF and VEGF release contributing to development of intrapulmonary vascular dilatation(IPVD) , and neoangiogenesis leading to anatomical shunt resulting decreased oxygenation. Sphingosine 1 phosphate (S1P) is an essential compound produced and secreted by endothelial cells, platelets and RBC's. S1P prevents adhesion, transmigration and release of inflammatory mediators from macrophages. S1P levels are decreased in cirrhotics. Simvastatin, a HMG CoA inhibitor has many pleotropic effects, Of which one is by agonizing the S1P response and improving oxygenation in HPS patients. Simvastatin at a optimal dose of 40mg/day for 6months. Pre and post simvastatin treatment related oxygenation changes and concurrently its effect on liver fibrosis will be evaluated.


Description:

Methodology: - Study population:All the consecutive patients of cirrhosis admitted to Hepatology department of ILBS will be evaluated for inclusion. - Study design: Double Blind randomized control trial: Superiority trial. The study will be conductedin Department of Hepatology ILBS. - Study period: 2 years - Sample size: - Assuming 40% as the response rate to simvastatin and 1% to standard medical treatment with α 5% , power 80% and superiority marging as 10% ,we need to enroll 36 cases 18 in each arm.Further considering 10% drop rate, decided to enroll 40 cases with 20 randomised to 2 groups using block randomisation method taking block score of 4.It is decided to allocate the cases in 2:1 ratio (Simvastatin 2: 1 Placebo) decided to enroll 45 cases so that 30 in simvastatin arm and 15 in standard medical therapy (Not on pentoxiphylline) arm with block size 15 - Intervention: - Patients to be divided into 2 groups - Group A-Simvastatin 40mg OD plus standard treatment - Group B-Matched placebo plus standard treatment (excluding Pentoxiphylline) - Stopping-rule-Development of drug related side effects - Disease progression (Increase in baseline MELD by 4 or >25) - Monitoring and assessment - Patients with known cirrhotics will be enrolled as per inclusion criteria and baseline routine testing with complete blood count, liver and kidney function test, ultrasonography of the abdomen, lipid profile, total CPK, measurement of liver and splenic stiffness.Pulmonary blood at the time of HVPG for endothelin-1 and TNF alpha,Nitric oxide levels,S1P expression,KLF-2 levels. - Matched placebo not on pentoxiphylline are included. - MELD score and Child score, Arterial blood gas analysis, Pulmonary function test,6 minute walk test,Saline contrast 2D ECHO at baseline and at 6months. - Clinical evaluation done monthly. Response at the end of 6months. - Hepatic venous pressure gradient (HVPG): - Prior to the HVPG measurement, a venous access was performed under ultrasonography after local anesthesia. The Seldinger technique was used to insert a catheter into the right brachial vein or the right internal jugular vein. An occlusion balloon catheter of 6 F was guided in a branch of the hepatic veins, usually the median or right vein, under fluoroscopic control and continuous electrocardiographic and pressure monitoring. - After inflating the balloon at the catheter's tip (maximum diameter ranges from 8.5-11.5 mm), a venous check was performed to demonstrate complete vessel occlusion. The wedged hepatic vein pressure (WHVP) was measured in this condition. Following that, the free hepatic vein pressure (FHVP) was measured after deflating the balloon at the catheter's tip. On a multi-channel recorder, a permanent trace was obtained. Pressures were also achieved in the inferior vena cava and the right atrium. According to the Baveno VI consensus, the HVPG-response was defined as a 20% or 12 mmHg reduction in HVPG after NSBB treatment. - HVPG= WHVP - FHVP (Normal is <5mm of Hg) - Ultrasonography of the abdomen: - dilated portal vein (>13 mm): non-specific - biphasic or reverse flow in portal vein (late stage): pathognomonic - recanalization of paraumbilical vein: pathognomonic - portal-systemic collateral pathways (collateral vessels/varices) - splenomegaly - ascites - The damping index (showing changes in the doppler hepatic vein waveform) corresponds with hemodynamically significant portal hypertension and HVPG values (together with HVPG changes after treatment) - splenic arterial resistive index Liver and splenic stiffness: - A 3.5-MHz ultrasound transducer probe is mounted on the axis of a vibrator in the FibroScan device. Mild amplitude, low-frequency (50 Hz) vibrations are transmitted to the liver tissue, causing an elastic shear wave to propagate through the underlying tissue. If the success rate was greater than 60% and the interquartile range (IQR) was greater than 30% of the median value, LS values were accepted. - Guidelines for measuring SS is same as LS. SS was performed on a supine patient with maximal abduction of the left arm, with the probe positioned in an intercostal space where the spleen was correctly visualized by US. Furthermore, in accordance with the FibroScan's technical features, patients with a splenic parenchymal thickness of >4 cm under the probe were excluded. - STATISTICAL ANALYSIS: - For comparison of parameters pretherapy and posttherapy, the Wilcoxon signed rank test was used. P.05 was considered significant. SPSS version 15.0 statistical software (SPSS Inc, Chicago, Illinois) was used for analysis. - Adverse effects: - 1. Major Sideeffects of Simvastatin - Rhabdomyolysis(Raised Total CPK > 3ULN) - Bradycardia - Transaminitis (ALT >5ULN) - Headache - Constipation - Upper respiratory tract infection 2. HVPG related complications - Transient arrhythmias - Vagal reaction - Local access pain and bleeding - Stopping rule : - Development of serious adverse effects leading to withdrawal of the drug or death from any cause. - Disease progression (Increase in baseline MELD by 4 or >25)


Recruitment information / eligibility

Status Recruiting
Enrollment 45
Est. completion date October 2023
Est. primary completion date October 2023
Accepts healthy volunteers No
Gender All
Age group 18 Years to 70 Years
Eligibility Inclusion Criteria: 1. Diagnosed case of Hepato-pulmonary syndrome AaPO2 > 15 mm Hg on standing room air arterial blood gas (ABG). PaO2<80 mmHg for clinical HPS between 18-70 years of years 2. Child A/B cirrhosis, Child C with CTP score of =/<10 3. Patient with no liver transplant option Exclusion Criteria: 1. Child-C cirrhosis CTP >10 2. Very Severe HPS 3. Acute-on-chronic liver failure 4. Thrombosis of splenoportal axis 5. Hepatocellular carcinoma 6. Renal dysfunction 7. Patients intolerant to beta blockers (history of hypotension or bradycardia) 8. Contraindication for beta-blockers (history of chronic obstructive pulmonary disease, atrioventricular block) 9. Pregnant females 10. Refusal to participate in the study 11. Hepatic Hydrothorax

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Simvastatin 40mg
Simvastatin 40mg OD
Other:
Placebo
Placebo
Standard medical Treatment
Standard medical Treatment eccluding pentoxiphylline

Locations

Country Name City State
India Institute of Liver & Biliary Sciences New Delhi Delhi

Sponsors (1)

Lead Sponsor Collaborator
Institute of Liver and Biliary Sciences, India

Country where clinical trial is conducted

India, 

Outcome

Type Measure Description Time frame Safety issue
Primary Achievement of complete response by the end of 6 months 6 months
Secondary Transplant free survival 3 months
Secondary Transplant free survival 6 months
Secondary Severity of Liver Disease Severity will be assess by MELD Na (Model for End Stage Liver Disease) 6 months
Secondary Development of serious adverse effects leading to withdrawal of the drug or death from any cause. 2 years
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