Hepatitis B Clinical Trial
Official title:
Study to Compare Virological Response to 0.5 mg Daily Versus 1.0 mg Daily Oral Doses of Entecavir in Chronic Hepatitis B Virus Infection Related Decompensated Cirrhosis
Entecavir (ETV) and tenofovir (TDF) are the first-line drugs for treatment of chronic
hepatitis B virus (HBV) infection. Chronic HBV infection gradually progress to liver
cirrhosis. Over time, as liver damage and cirrhosis advance, the illness progress to a stage
termed as decompensated cirrhosis, characterized by development of one or more of serious,
life-threatening complications (ascites, hepatic encephalopathy, variceal bleeding or
jaundice). In HBV related decompensated cirrhosis, antiviral treatment is shown to provide
benefit.
For HBV related decompensated cirrhosis, EVT is the drug of choice as it has been shown to be
effective and safe. The usual dose of ETV for chronic HBV infection is 0.5 mg orally once
daily. Somehow, the recommended dose of ETV for decompensated cirrhosis has been 1.0 mg/d.
The literature provides no justification for using this double dose of ETV. Since 0.5 mg
daily works well in other stages of disease, there is little reason why it should not work
well even in treatment-naïve decompensated cirrhosis. Considering the limitations of
available literature, physicians' are divided in their opinion about the drug dose and are
prescribing either of the two doses of ETV for this group. Hence, there is a need to assess
whether the usual 0.5 mg/d of ETV would work as well as the 1.0 mg/d dose of ETV in
decompensated cirrhosis due to HBV infection.
Investigators planned this open-labeled observational study with objective to compare the
efficacy of HBV suppression achieved using 0.5 mg daily and 1.0 mg daily of ETV in
HBV-related decompensated cirrhosis by comparing the mean reduction in HBV DNA level from
baseline after 24 weeks of treatment.
In present study investigators propose to enroll 15 participants in each group who has been
started on either doses (0.5 mg and 1.0 mg) of entecavir and measure serum HBV DNA levels in
blood specimens (5 ml) will be collected at different time points, i.e. at baseline, 2, 4, 8,
12 and 24 weeks after starting entecavir.
Background Chronic infection with hepatitis B virus (HBV), if untreated, may progress to
liver cirrhosis, portal hypertension and hepatocellular carcinoma. Currently, oral
administration of one of the nucleos(t)ide analogues (NAs) is the preferred treatment for
chronic HBV infection. Of the five NAs approved for HBV treatment, lamivudine, adefovir and
telbivudine are no longer preferred, and the recent guidelines from all three major
international liver disease associations [American Association for the Study of Liver Disease
(AASLD), European Association for Study of Liver (EASL), and Asia-Pacific Association for
Study of Liver (APASL)] recommend the use of either entecavir (ETV) or tenofovir (TDF) as
first-line drugs, because of their lower propensity to induce drug-resistant mutants and
hence better efficacy.
Chronic liver disease due to any cause gradually progress to liver cirrhosis. Over time,
liver damage and cirrhosis advances to a stage termed as decompensated cirrhosis,
characterized by development of one or more of serious, life-threatening complications
(ascites, hepatic encephalopathy, variceal bleeding or jaundice). Treatment of HBV infection
with anti-viral drugs, in presence of decompensated cirrhosis, is beneficial.
In presence of HBV-related decompensated cirrhosis, EVT is the drug of choice as it has been
shown to be effective and safe. The usual dose of ETV for chronic HBV infection is 0.5 mg
orally once daily. Somehow, the recommended dose of ETV in presence of decompensated
cirrhosis has been 1.0 mg/d. The literature provides little direct justification for using
this double dose of ETV. Possibly, initially, ETV was used empirically in this dose to
achieve a rapid HBV suppression in this high-risk group with prior exposure to lamivudine in
advanced liver disease. However, since 0.5 mg daily works well in other stages of disease,
there is little reason why it should not work well even in treatment-naïve decompensated
cirrhosis. On the other hand, use of this higher dose of ETV adds to cost, a major
consideration in areas where medical expenses are mostly met with out of the pocket expenses.
Hene, in view of above-mentioned limitations of available literature, opinion of physicians
is divided and either of the two doses of ETV is used in HBV related decompensated cirrhosis.
Hence, there is a need to assess whether the usual 0.5 mg/d of ETV would work as well as the
1.0 mg/d dose of ETV in decompensated cirrhosis due to HBV infection.
Hypothesis
Entecavir treatment in a dose of 0.5 mg once daily and of 1.0 mg daily have comparable
antiviral efficacy in HBV-related decompensated cirrhosis.
Objective
To compare the efficacy of HBV suppression achieved using 0.5 mg daily and 1.0 mg daily of
ETV in HBV-related decompensated cirrhosis by comparing the reduction in HBV DNA level from
baseline till up to 24 weeks of treatment.
Study design
Open-label administration of 0.5 mg or 1.0 mg daily of entecavir for 24 weeks with comparison
of mean reduction in HBV DNA levels from baseline in participants receiving the two dose
schedules.
Study subjects
Participants with decompensated liver cirrhosis and replicative HBV infection (HBsAg
positive, serum HBV DNA titer >100,000 IU/mL) will be enrolled, irrespective of their HBeAg
and anti-HBe test results. Diagnosis of cirrhosis will be based on a combination of typical
clinical, biochemical, radiological and endoscopic findings. Hepatic decompensation will be
defined according to the most recent definition of APASL which defines it as significant
liver dsyfunction as indicated by (i) raised serum bilirubin (more than 2.5 times the upper
limit of normal) and prolonged prothrombin time (prolonged by more than 3 s or international
normalized ratio >1.5) or (ii) occurrence of ascites or (iii) hepatic encephalopathy.
Participants with one or more of the following features will be excluded: (i) prior exposure
to NAs or other specific treatment for HBV infection (e.g. pegylated interferon), (ii)
hepatocellular carcinoma, (iii) co-infection with any other hepatotropic viruses or HIV, (iv)
acute-on-chronic liver failure as defined by the criteria laid down by Asia-Pacific
Association for the Study of Liver, (iv) significant alcohol intake or another concomitant
hepatobiliary disease, (v) expected survival below 4 weeks (e.g. hemodynamic instability,
active sepsis, hepatorenal syndrome, etc), (vi) use of immunosuppressive medication or (vii)
portal vein thrombosis. Also, a participant who is not in a position to return for the
scheduled follow-up visits will be excluded.
Study procedures
Enrollment and consent
We will consider to enroll the participants with HBV related decompensated cirrhosis and is
planned for treatment, based on their clinical conditions, with either 0.5 or 1.0 mg daily
doses of Entecavir by their treating physician. For those who agree to participate (by
signing an informed consent), clinical and laboratory findings (including baseline HBV DNA
level) will be recorded.
Follow-up and outcome measure
Blood specimens (5 ml) will be collected at different time points, i.e. at baseline, 2, 4, 8,
12 and 24 weeks after starting Entecavir. Serum will be separated and stored at -80C till
analysis. In each specimen, HBV DNA will then be assessed using a quantitative real-time PCR.
Sample size
It is proposed to enroll 15 participants in each arm.
Data analysis
The rate of decline in HBV DNA levels with time will be compared between groups, using
methods for longitudinal data analysis.
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