Hepatitis B, Chronic Clinical Trial
Official title:
A Randomized, Open-label, Single-dose, Two-period, Crossover Study to Demonstrate the Bioequivalence of the Fixed Dose Combination (FDC) of Lamivudine and Adefovir Dipivoxil (100mg/10mg) to Heptodin® (100mg ) and Hepsera® (10mg)
This is a phase I study being conducted to support the clinical development program of a FDC
product of the nucleoside analogue lamivudine and the nucleotide analogue adefovir dipivoxil.
To establish bioequivalence, the exposure of lamivudine and adefovir dipivoxil when
administered as the FDC will be compared to that of Heptodin (lamivudine) and Hepsera
(adefovir dipivoxil) when administered separately. In this study, the FDC product will
contain 100mg lamivudine/10mg adefovir dipivoxil.
Total 40 healthy adult subjects will be enrolled. The study will include a screening visit
and two treatment sessions. The screening visit will be conducted up to 3 weeks prior to the
first dose of Session 1. All subjects will receive Regimen A through B according to the
randomization schedule. Eligible subjects will be enrolled in the study and randomized to
receive the following treatment regimens in table below in one of the following treatment
sequences: AB, or BA. There will be a seven to ten days washout period between each treatment
session. Pharmacokinetic sampling for measurement of plasma lamivudine and adefovir dipivoxil
concentrations will be conducted over a 48-hour period following the morning administration
of study medication in each study session. During this time, all subjects will remain in the
unit for pharmacokinetic (PK) sample collection. The total duration (from screening to the
end of the study) of each subject's participation will be approximately four weeks.
Chronic hepatitis B (CHB) infection is common, with an estimated global prevalence of more
than 400 million people, or approximately 5% of the world's population. Chronic hepatitis B
virus (HBV) carriers with evidence of ongoing viral replication are at highest risk for the
development of active liver inflammation (i.e., hepatitis B) and progressive liver disease.
They are also the major contributor to the spread of HBV infection.
The goals of therapy in CHB include suppression of HBV replication, reduction of
necroinflammatory processes in the liver, and prevention of progression to serious liver
disease or death. The HBV polymerase has an error rate that is intermediate between that of
human immunodeficiency virus (HIV) and herpes virus polymerases,; this predicts that patients
with CHB infection are likely to exhibit some degree of antiviral resistance to nucleoside or
nucleotide monotherapies. Indeed, patients on long-term lamivudine therapy have been found to
have HBV variants (YMDD variants) with reduced sensitivity to lamivudine in vitro, and have
exhibited variably diminished therapeutic responses.
A fixed dose combination (FDC) formulation of lamivudine and adefovir dipivoxil for the
treatment of CHB. Lamivudine (Heptodin) an active triphosphate (3TC-TP) incorporating into
growing DNA chains results in premature chain termination thereby inhibiting HBV DNA
synthesis. Adefovir dipivoxil (Hepsera) is an orally bioavailable pro-drug of adefovir, a
nucleotide analog of adenosine monophosphate. It can inhibit both the reverse transcriptase
and DNA polymerase activity and is incorporated into HBV DNA causing chain termination.
A FDC would therefore combine the established benefits of two important anti-HBV antiviral
drugs, representing the first combination product for the treatment of CHB. In addition to
the enhanced efficacy afforded by combination therapy, the use of a combination product could
enhance convenience and compliance and ensure that patients receive the two drugs needed.
This study will evaluate the bioequivalence of a FDC containing (lamivudine 100 mg/adefovir
dipivoxil 10 mg) compared to Heptodin100 mg and Hepsera 10 mg. This dose was selected as both
Heptodin 100 mg and Hepsera 10 mg are approved in the PRC for the treatment of CHB. Based on
extensive clinical experience with the use of both drugs either as monotherapy or in
combination, it is anticipated that the co-administration of both agents in the FDC
formulation will be well-tolerated.
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