Hepatitis B Clinical Trial
Official title:
Lamivudine and Therapeutic Vaccine Evaluation in Senegalese Patients With Chronic Hepatitis B Infection
Chronic hepatitis B infection is a major public health issue in Senegal. The study will compare the efficacy of the treatment strategy combining Lamivudine and therapeutic vaccine (12 intra-muscular injections over a 6-month period) to a treatment with Lamivudine alone on the control of viral replication in patients with a replicative hepatitis B virus (HBV) infection and an increase in hepatic enzymes.
Hepatitis B infection with a prevalence higher than 15% of positive Ag HBs subjects is a
major public health issue in Senegal. A program of treatment of patients presenting with
hepatic disease is currently ongoing through a network of specialists in GI tract and liver
diseases. Hepatitis B is a real threat in the Senegalese population as showed in a pilot
study (HEPADAK I) performed at the Dakar Hospital Principal (DHP) in Dakar among 100 blood
donors and 50 patients with liver disease. This study allowed us to better characterize the
strains at the molecular level. The aim of the project is to assess a pragmatic treatment
strategy which can be applied to Senegal or other developing countries for patients
requiring treatment. A recent Japanese study performed in Ag HBe positive patients reported
the interest of the combination of Lamivudine (LAM) and a therapeutic vaccine with the
negativation of viral load in 100% of patients after one year of treatment. It is important
to show that such a treatment with 12 intra-muscular injections of the vaccine over a
6-month period is feasible in Africa and to assess the results of such a treatment in the
Senegalese population, which is mainly AgHBe negative.
The study HEPADAK 2 is a randomized open label study which will compare the efficacy of the
treatment strategy combining Lamivudine and therapeutic vaccine (12 intra-muscular
injections of Engerix B over a 6-month period) to a treatment with Lamivudine alone on the
control of viral replication in patients with a replicative HBV infection and an increase in
transaminases.
Eligible patients have to be HIV, HDV and HCV negative and will have to i) give their
written informed consent; ii) have a B hepatitis grade over or equal to F2 with the Metavir
score, DNA HBV greater than 105 copies/mL (or 104 copies/mL if Ag Hbe -) , ALAT greater than
1.3 times the upper limit of the normal; iii) accept to have a liver biopsy and to be
followed for this protocol at the DHP. After a 3-month treatment with Lamivudine, patients
whose viral load is negative or at least decreased by 4 Log will be randomized to the same
treatment for a further 9-month period or to the same treatment combined with 12 injections
of vaccine over 6 months. The main endpoints are undetectability of HBV DNA blood level 12
months after treatment initiation and 6 months after the end of the treatment. Secondary
endpoints will be HBV DNA blood levels at 3, 6, 9 and 12 months after the end of the
treatment, transaminases blood level, Lamivudine treatment compliance, the feasibility of
the vaccine injections schedule, safety, AgHBe seroconversion (in positive patients) and
negativation of AgHBs. Two hundred ten patients have to be included (70 in the Lamivudine
group, and 140 in the Lamivudine + vaccine group) in order to show a difference of at least
20% in the percentage of patients with an undetectable viral load at 12 months (70% expected
under Lamivudine monotherapy), with a power of 90%, an alpha risk equal to 5% and a
bilateral test. Patients with a virological failure will be maintained or retreated with
Lamivudine. For the patients with an YMDD mutation, a treatment with Adefovir Dipivoxil will
be possible. Patients' inclusion is planned to start in January 2005 and end after 12 or 18
months. Patients will be treated during one year and followed one year without treatment in
the study protocol, and then will be managed if necessary
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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