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NCT04431375 Clinical Trial

Efficacy of Addition of Fecal Microbiota Transplant (FMT) and Plasma Exchange to Tenofovir in Comparison to Monotherapy With Tenofovir in ACLF-HBV

Hepatitis B Clinical Trial

Official title:
Efficacy of Addition of Fecal Microbiota Transplant (FMT) and Plasma Exchange to Tenofovir in Comparison to Monotherapy With Tenofovir in ACLF-HBV

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT04431375
Other study ID # ILBS-ACLF-05
Secondary ID
Status Recruiting
Phase N/A
First received
Last updated
Start date June 22, 2020
Est. completion date June 10, 2022

Study information
Verified date January 2022
Source Institute of Liver and Biliary Sciences, India
Contact Dr G. Srinivasa Reddy, MD
Phone 01146300000
Email srinivasareddygolamari@gmail.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

A randomized controlled trial to study the efficacy of addition of FMT & plasma exchange to tenofovir compared to monotherapy with tenofovir in patients with HBV reactivation who develops Acute on chronic liver failure. In this study the patients who meet the inclusion criteria will be randomized to either receive Tenofovir or with FMT + plasma exchange along with Tenofovir . Blood samples & stool samples will be taken & analysis will be done accordingly .The patients are followed for 90 days MELD,APACHE & SOFA scores are calculated.Then statistical analysis will be done to find whether the addition of plasma exchange & FMT adds benefit compared to tenofovir treatment alone .

Description:

A randomized controlled trial to study the efficacy of addition of FMT & plasma exchange to tenofovir compared to monotherapy with tenofovir in patients with HBV reactivation who develops Acute on chronic liver failure. In this study the patients who meet the inclusion criteria will be randomized to either receive Tenofovir or with FMT + plasma exchange along with Tenofovir . Blood samples & stool samples will be taken & analysis will be done accordingly .The patients are followed for 90 days MELD,APACHE & SOFA scores are calculated.Then statistical analysis will be done to find whether the addition of plasma exchange & FMT adds benefit compared to tenofovir treatment alone . Study period: 2 Years Intervention: The patients in Group A will receive T.Tenofovir [antiviral] 300mg per oral once a day . The patients in Group B will receive Plasma exchange 2 sessions alternate day followed by FMT for 7 days and Tenofovir [antiviral] 300mg PO once a day . Intravenous antibiotics will be given to all patients included in study empirically, because of high risk of infection in these patients. Patients with sepsis are excluded from the study. Methodology for FMT - Fresh Stool [30 g] is obtained from donor <3 hr before FMT. 150 mL sterile 0.9N saline is added to sample & homogenized in a blender. It is Continued 3 times in pulses of 20-30 secs, till homogenous suspension. Slow filtration is done with membrane filter (330µm) to give adequate time. Filtration is repeated 3 times. Patient is kept NPO for 4 hrs. prior to the instillation .100 ml of fresh filtrate is given for 7 days through naso-jejunal tube over 5-10 minutes .Patient is kept reclined at 45° for 4 hr. Normal diet is given after 2 hr of procedure. IV antibiotics are continued as per institutional protocol in case of sepsis. Methodology for plasma exchange [PE] - Circulatory access will be established through a double lumen catheter via the patient's femoral vein. The total exchanged plasma volume will be 2500-3500 mL, and the Plasma Exchange rate will be 20-25 mL/min. Fresh-frozen plasma (FFP) will be supplied by the ILBS Blood Bank. Dexamethasone (5 mg) and heparin (2500 U) will be injected routinely before PE. Heparin will be neutralized at the end of PE by an injection of 20-50 mg protamine sulfate. PE will be repeated alternate day for a total of 2 sessions Adverse effects: FMT FMT - Sore throat and difficulty in deglutition secondary to naso-gastric tube insertion Plasma exchange PE - Hypocalcemia - Hypokalemia - Metabolic alkalosis - Hypotension - Anaphylaxis - TRALI TENOFOVIR Tenofovir - Reversible proximal renal tubular toxicity. - Reduced bone mineral density - Manifestations of mitochondrial toxicity (i.e., neuropathy, myopathy, lactic acidosis Stopping rule of study: - Allergic reactions except mild drug reactions - Arterial hypotension or development of shock /Hypertension - Arrhythmias - Development or progression of organ failures during therapy - Transfusion related lung injury - Uncontrolled Bleeding or DIC - Severe dyselectrolytemia( k+<2.5 or >5.5) - Seizures/tetany - Patients who are undergoing or listed for Transplantation

Recruitment information / eligibility
Status Recruiting
Enrollment 70
Est. completion date June 10, 2022
Est. primary completion date June 10, 2022
Accepts healthy volunteers No
Gender All
Age group 18 Years to 75 Years
Eligibility Inclusion Criteria: - Age - 18-75 years - Patients with ACLF - HBV reactivation according to APASL guidelines. - MELD < 30 WITH AKI,HE - MELD < 30 WITH OUT EXTRAHEPATIC FAILURE Exclusion Criteria: - MELD > 30 - Co existing hepatitis A,E,D - HCC - Sepsis - Alcohol intake, substance abuse, HIV, IBD, chronic constipation or diarrhoea - Allergy to plasma, protamine or heparin, - Active hemorrhage or disseminated intravascular coagulation (DIC) - Unstable hemodynamics (e.g., blood pressure <90/60 mmHg, heart rate >100 bpm), - Cerebral or myocardiac infarction - Pregnancy

Study Design

Related Conditions & MeSH terms

Intervention

Biological:
Plasma Exchange
Plasma exchange 2 sessions alternate day followed by FMT for 7 days and Tenofovir [antiviral] 300mg PO once a day .
Drug:
Tenofovir
Tenofovir [antiviral] 300mg PO once a day .
Other:
Fecal Mircobiota Transplantation
FMT for 7 days

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 Overall survival in both groups Day 28
Secondary Overall survival in both groups 3 months
Secondary Reduction in HBV DNA level 14 days
Secondary Reduction in HBV DNA level 60 days
Secondary Reduction in HBV DNA level 90 days
Secondary Reduction in CTP Score in both groups CTP Score ranges from 5 to 15 5=good 15=worst 14 days
Secondary Reduction in CTP Score in both groups CTP Score ranges from 5 to 15 5=good 15=worst 30 days
Secondary Reduction in CTP Score in both groups CTP Score ranges from 5 to 15 5=good 15=worst 60 days
Secondary Reduction in CTP Score in both groups CTP Score ranges from 5 to 15 5=good 15=worst 90 days
Secondary Reduction in MELD Score in both groups MELD Score ranges from 6 to 40 6=good 40=worst 14 days
Secondary Reduction in MELD Score in both groups MELD Score ranges from 6 to 40 6=good 40=worst 30 days
Secondary Reduction in MELD Score in both groups MELD Score ranges from 6 to 40 6=good 40=worst 60 days
Secondary Reduction in MELD Score in both groups MELD Score ranges from 6 to 40 6=good 40=worst 90 days
Secondary Percentage of patient's with improvement in hepatic failure calculated by MELD Na and CTP scores. 14 days
Secondary Percentage of patient's with improvement in hepatic failure calculated by MELD Na 30 days
Secondary Percentage of patient's with improvement in hepatic failure calculated by CTP scores. 30 days
Secondary Percentage of patient's with improvement in hepatic failure calculated by MELD Na 60 days
Secondary Percentage of patient's with improvement in hepatic failure calculated by CTP scores. 60 days
Secondary Percentage of patient's with improvement in hepatic failure calculated by MELD Na. 90 days
Secondary Percentage of patient's with improvement in hepatic failure calculated by CTP scores. 90 days
Secondary Change in microbiota profile in both groups 10 days
Secondary Change in microbiota profile in both groups 30 days
Secondary Change in microbiota profile in both groups 60 days
Secondary Change in microbiota profile in both groups 90 days
Secondary Change in plasma cytokine profile in both groups 10 days
Secondary Change in plasma cytokine profile in both groups 28 days
Secondary Change in plasma cytokine profile in both groups 60 days
Secondary Number of patients with adverse Events in both groups 90 days
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