Hepatitis B Clinical Trial
Official title:
Combination of Lamivudine and Adefovir Dipivoxil for Treatment of Chronic Hepatitis B
This study will evaluate the safety and effectiveness of lamivudine plus adefovir versus
adefovir alone to treat chronic hepatitis B infection. The Food and Drug Administration has
approved lamivudine for the treatment of hepatitis B. However, the drug is not effective in
all patients, and many of those in whom it initially works develop resistance after 1 to 3
years. Adefovir is an experimental drug that inhibits replication of the hepatitis B virus
(HBV). Adefovir used alone may be adequate to provide sustained suppression of the virus and
improvement in liver disease. However combining two anti-viral agents may be superior to
using one alone, similar to the strategy employed for the treatment of AIDS. This study will
test whether the combination of lamivudine and adefovir is better than adefovir alone for
the treatment of chronic hepatitis B.
Patients 18 years of age and older, who have been infected with HBV for at least 6 months,
may be eligible for this study. Candidates may not have received lamivudine treatment in the
past 6 months or prior treatment with adefovir and must not be taking other anti-viral
treatments for their hepatitis. They will have a blood test to confirm HBV infection.
Participants will be admitted to the NIH Clinical Center for 2 to 3 days for a medical
evaluation. One to 2 weeks after the evaluation, patients will be randomized to begin taking
lamivudine and adefovir, or adefovir alone. Therapy will continue for at least 12 months.
Follow-up clinic visits will be scheduled weekly for the first month, then every 4 to 8
weeks for the rest of the treatment period. Patients will be evaluated at the end of 1 year.
Patients who have not improved with treatment will stop taking the treatment and will be
evaluated in the clinic once every 4 weeks for another 6 months. Patients who show an
improvement in their liver injury may continue taking lamivudine and adefovir or adefovir
alone for 4 more years, as long as they continue to improve with the medication. Progress
will be evaluated. If the test results show no continued improvement or are negative for
hepatitis B antigens, therapy will be stopped.
Patients who continue treatment for 5 years will be readmitted at year 4 for another medical
evaluation to assess the effects of treatment at that time. After the 5 years all patients
will stop therapy at and be followed with regular clinic visits for at least 6 months.
Aims: To assess the safety, antiviral activity and clinical benefit of the combination of
lamivudine and adefovir dipivoxil vs adefovir alone in up to 80 patients with chronic
hepatitis B for up to five years.
Background: Adefovir dipivoxil and lamivudine are oral antiviral agents that have been shown
to have potent activity against HBV in vitro and in vivo. Both drugs have been used
extensively in patients with HIV infection and more recently in controlled trials as
monotherapy in patients with chronic hepatitis B. Lamivudine is currently approved as
therapy of hepatitis B and has been evaluated extensively both as a one-year course of
treatment as well as long-term continuous therapy. While lamivudine monotherapy induces a
transient improvement in viral levels and liver histology, viral resistance develops in a
large proportion of patients with re-appearance of HBV DNA in serum in high levels
associated with mutations in the Tyrosine-methionine-aspartate-aspartate (YMDD) motif of the
HBV polymerase gene and worsening of the hepatitis. Adefovir monotherapy, in contrast, has
not been shown to be associated with development of viral resistance even when given for up
to two years. When given as monotherapy for 1 year, adefovir leads to improvement in
histology of hepatitis B in approximately 50% of patients. At present, the long-term
efficacy of adefovir has not been shown.
Protocol: Up to 80 patients with chronic hepatitis B who have raised serum ALT (alanine
aminotransferase) levels, HBV DNA in serum (above 1 million copies per ml by quantitative
PCR) and active liver disease on liver biopsy will be enrolled and started on the
combination of lamivudine (100 mg daily) and adefovir dipivoxil (10 mg daily) or adefovir
alone (10 mg daily). Patients will be stratified into one of four groups of 20 patients for
randomization: (A) Lamivudine naive and HBeAg positive, (B) Lamivudine naive and HBeAg
negative (C) previous lamivudine therapy and HBeAg positive and (D) previous lamivudine
therapy and HBeAg negative. Patients will be monitored carefully during therapy for adverse
events, clinical symptoms and signs of liver disease, biochemical, and hematological
parameters, and HBV serology at 2 to 4 week intervals. The primary endpoint of therapy will
be a maintained combined response (a combination of virological, biochemical, and
histological response) with major timing of end-points being at 1 and 4 years. Secondary
endpoints will include loss of HBeAg, the individual types of maintained responses
(virological, biochemical and histological), the development of lamivudine resistance, and
improvement in symptom scores and quality of life assessments at 1 and 4 years.
Conclusions: This study will assess the effects of the combination of lamivudine and
adefovir dipivoxil compared to adefovir alone in suppressing hepatitis B and prevention of
lamivudine resistant mutants that arise during long-term therapy with lamivudine alone.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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