Chronic Hepatitis B Clinical Trial
Official title:
Pegasys Plus Entecavir Versus Entecavir Alone for Hepatitis Be Antigen-Positive Chronic Hepatitis B
Although the best treatment choice for chronic hepatitis B is not clarified yet, certain
therapeutic concepts could be derived from the experience of treating patients with chronic
hepatitis C or human immunodeficiency virus (HIV) infection. A major advancement in treating
hepatitis C or HIV infection has been the development of combination therapy. Whether the
combination therapy using Peg-IFN alfa-2a plus ETV can achieve a long-term beneficial effect
against ETV alone is not clarified. A prior single-arm pilot study suggested that similar
combination therapy may be beneficial in patients with chronic hepatitis B. In this
proposal, we thus hypothesize that the efficacy by using combination therapy with pegylated
IFN alfa-2a plus ETV is superior to that by using ETV alone in that Peg-IFN may restore host
immunity against HBV and prolonged ETV can maximize viral suppression.
The objective of this clinical trial is to evaluate the efficacy of the combination of
Peg-IFN alfa-2a at a dose of 180 mcg administered subcutaneously per week and ETV 0.5 mg
daily for 24 weeks followed by ETV 0.5 mg daily monotherapy for an additional 120 weeks
versus ETV 0.5 mg daily monotherapy for 144 weeks in patients with HBeAg-positive chronic
hepatitis B. It will be an open-label, randomized, comparative, multi-center clinical trial.
The recruited patients will be equally randomized into two treatment groups. Treatment-free
follow-up period will be 48 weeks in both groups of patients. All subjects will be assessed
for loss of HBeAg, presence of anti-HBe, loss of HBsAg, presence of anti-HBs, suppression of
HBV DNA, and normalization of serum ALT at the end of treatment and end of follow-up.
Genotypic and virologic resistance to ETV will also be assessed at baseline and at end of
years 1, 2 and 3. The primary efficacy will be HBeAg seroconversion.
Currently, there are several antiviral treatments effective for suppression of viral
replication but still failed to cure HBV infection in patients with chronic hepatitis B. The
short-term treatment goals are thus to control hepatitis activity, to obtain hepatitis B e
antigen (HBeAg) seroconversion, and to improve necroinflammatory activity and fibrosis of
the liver. Six drugs have been worldwide approved for the treatment of chronic hepatitis B
at present: conventional IFN (IFN) alfa, lamivudine (LAM), adefovir dipivoxil (ADV),
pegylated IFN (Peg-IFN) alfa, entecavir (ETV) and recently telbivudine (LdT). Conventional
IFN alfa monotherapy has a narrow range of efficacy, is associated with several adverse
effects and is inconvenient because of frequent injections. Lamivudine is better tolerated;
but virologic response to lamivudine is frequently not durable and prolonged lamivudine
treatment is commonly associated with the emergence of drug-resistant HBV mutants. Adefovir
dipivoxil is effective and has been approved for the treatment of chronic hepatitis B in
many countries, but is nephrotoxic at doses higher than 10 mg per day for long time.
Pegylated IFN alfa has been shown to be superior to conventional IFN alfa and lamivudine,
and has already been approved for the treatment of chronic hepatitis B. Overall,
satisfactory virologic and serologic responses could be achieved using pegylated IFN alfa
alone in around 30-44% of these patients. Entecavir, a carbocyclic deoxyguanosine analog,
which is active against both lamivudine- and adefovir dipivoxil-naïve and -resistant HBV, is
the most potent anti-HBV agent ever discovered. In addition, the 4-year drug resistance rate
is <1.0% in selected lamivudine-naïve patients. LdT is another thymidine nucleoside analogue
with potent in vitro activity against HBV and approved for CHB. Recent phase III GLOBE
trials have proved this agent to be more effective in the treatment of HBeAg+ve and -ve
chronic hepatitis B than lamivudine. However, resistance to telbivudine was noted in around
10% of subjects after 104-week continuous therapy, although still fewer than that in
patients receiving lamivudine.
Although the best treatment choice for chronic hepatitis B is not clarified yet, certain
therapeutic concepts could be derived from the experience of treating patients with chronic
hepatitis C or human immunodeficiency virus (HIV) infection. A major advancement in treating
hepatitis C or HIV infection has been the development of combination therapy. Whether the
combination therapy using Peg-IFN alfa-2a plus ETV can achieve a long-term beneficial effect
against ETV alone is not clarified. A prior single-arm pilot study suggested that similar
combination therapy may be beneficial in patients with chronic hepatitis B. In this
proposal, we thus hypothesize that the efficacy by using combination therapy with pegylated
IFN alfa-2a plus ETV is superior to that by using ETV alone in that Peg-IFN may restore host
immunity against HBV and prolonged ETV can maximize viral suppression.
The objective of this clinical trial is to evaluate the efficacy of the combination of
Peg-IFN alfa-2a at a dose of 180 mcg administered subcutaneously per week and ETV 0.5 mg
daily for 24 weeks followed by ETV 0.5 mg daily monotherapy for an additional 120 weeks
versus ETV 0.5 mg daily monotherapy for 144 weeks in patients with HBeAg-positive chronic
hepatitis B. It will be an open-label, randomized, comparative, multi-center clinical trial.
The recruited patients will be equally randomized into two treatment groups. Treatment-free
follow-up period will be 48 weeks in both groups of patients. All subjects will be assessed
for loss of HBeAg, presence of anti-HBe, loss of HBsAg, presence of anti-HBs, suppression of
HBV DNA, and normalization of serum ALT at the end of treatment and end of follow-up.
Genotypic and virologic resistance to ETV will also be assessed at baseline and at end of
years 1, 2 and 3.
We anticipate the rate of HBeAg seroconversion, primary efficacy parameter, to be around 35%
at the end of 3-year entecavir therapy, but decreases to be 30% at the end of 24-week
post-treatment follow-up. We also anticipate that by combining Pegasys, the rate of
seroconversion at the end of treatment is 50% and at the end of 24-week post-treatment
follow-up could be 45%. With a 5% nominal significance level (one-sided), 128 patients per
group under a 1:1 ratio (a total of 256 patients) will provide 80% power to detect a
difference of 15% in treatment response rates between group I and II. Because this will be a
4-year study for each patient, we thus anticipate that the dropout rate may be as high as
15%. Accordingly, a total of 294 patients will be recruited, in order to account for a
dropout rate of up to 15%.
A final analysis will be conducted when all patients have completed 144-week treatment and
48 weeks of follow-up. Primary and secondary efficacy parameters will be evaluated by an
intention-to-treat analysis. Exact (1-sided) 95%-confidence interval from the binomial
distribution will be provided for response rates in individual patient groups. All
categorical and continuous variables will be analyzed by chi-square test and Student t test,
respectively. For continuous variables with outliers, nonparametric test will be used
instead. The analysis of histologic response will include only those who receive the pre-
and post-treatment biopsy.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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