Chronic Hepatitis Clinical Trial
Official title:
Phase IV Study of the Efficacy of Entecavir in Patients With Chronic Hepatitis B Virus Infection and Persistently Normal Alanine Aminotransferase
Entecavir (ETV) has shown superior ability to suppress hepatitis B virus (HBV) replication, histology improvement as well as low rate of emergence of resistant mutants. Out of range of clinical recommendations for treatment of chronic hepatitis B (CHB), chronic HBV carriers with persistently normal ALT and viral load more than 10^5 copies/mL have progression of liver disease during long-term follow-up. In addition, certain proportions of these patients do have significant inflammation and fibrosis in liver histology. This study will be able to identify who are at risk of liver disease progression and evaluate efficacy of ETV regarding improvement of liver histology during short-term (1-year) and long-term ETV treatment (3-year).
TITLE : A Randomized, Double-blind, Placebo-control Study Evaluating the Efficacy of
Entecavir in Patients with Chronic Hepatitis B Virus Infection and Persistently Normal
Alanine Aminotransferase INDICATION : Chronic hepatitis B virus infection with persistently
normal ALT
OBJECTIVES :
Primary objective To evaluate the efficacy of entecavir (ETV) in improving liver histology
in patients with chronic hepatitis B virus infection and persistently normal ALT.
The primary endpoint is to compare the proportion of subjects in each treatment group who
achieve the histologic Endpoint, defined as improvement in the necroinflammatory score (≥ 2
point decrease in Knodell HAI score) and no worsening of fibrosis (≥ 1 point increase in the
Knodell fibrosis score), at the Week 52 compared to baseline.
Secondary objectives
To compare the proportion of subjects in each treatment group with the following objectives
at week 52, week 104, and week 156, and post-dosing 24 weeks:
1. Undetectable HBV DNA by the Roche TaqMan® HBV Test (limit of detection 60 IU/mL); HBV
DNA by PCR will also be evaluated as a continuous parameter;
2. The reduction of HBV DNA from baseline.
STUDY DESIGN This is a 3-year prospective randomized, double-blind, placebo-control study.
Enrolled subjects will be allocated according to HBeAg status (HBeAg-positive and
HBeAg-negative), then randomized to ETV or placebo group.
ETV group: 1st year: ETV 0.5mg qd, then open with ETV 0.5mg qd for 2nd, 3rd year Placebo gr:
1st year: placebo, then open with ETV 0.5mg for 2nd, 3rd year
Dose of ETV: 0.5 mg/day Screening period: 6 weeks Timing of liver biopsy: baseline, 52th
week, 156th week NUMBER OF PATIENTS 130 (1:1)
STUDY PERIOD NOV 2007 ~ MAY 2011 DRUG ADMINISTRAITON Route: oral Dose: ETV 0.5 mg/day
Comparable placebo
STATISTICAL ANALYSIS Sample size determination:
An evaluation of the efficacy of entecavir compared to placebo is planned. A test for
superiority of entecavir to placebo will be conducted that has high power to demonstrate
superiority if there are larger histologic improvements of clinical importance. Histologic
improvement after one year is estimated as 50% of entecavir treatment and 25% of placebo.
Thus, a sample size of 47 will be required for 90% of confidence level with 5% of error.
Finally, we estimate that it will be appropriate to enroll 65 patients in each arm due to
probably patients' withdrawal.
Statistical Analyses The difference in response rates for the Histologic Endpoint
(entecavir-placebo) along with its standard error and 95% confidence interval will be
computed. Subset analyses defined by prognostic variables [e.g. gender, and HBV DNA level]
for the Histologic Endpoint will be performed.
Change from baseline at Week 52 and 156 in Knodell Scores will also be summarized as a
continuous parameter. The secondary efficacy variables will also be summarized and compared
between the treatment groups.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Treatment
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