|
The
Lancet Publishes First Study Showing Peginterferon Alfa-2b Is
Effective As Monotherapy In the Treatment of Chronic Hepatitis B:
Press Announcement from the Erasmus Medical Center
The
Erasmus Medical Center (EMC) in Rotterdam, The Netherlands today
issued a press release on the results of an international clinical
study published in this week’s issue of The Lancet (1).
The study showed that peginterferon
alfa-2b (Peg Intron) produced sustained
responses in patients with chronic hepatitis B. Following is
the text of the EMC announcement:
“The investigator-initiated study is
the largest clinical trial to date with peginterferon
alfa-2b therapy for chronic hepatitis B. “Our study showed that
patients with chronic hepatitis B responded to peginterferon alfa-2b,
and achieved higher sustained response rates than is typically seen
with any other antiviral treatment,” said lead investigator Harry
Janssen, M.D., Ph.D., from the Erasmus Medical Center in Rotterdam,
The Netherlands, where the international study was coordinated.
“Based on our findings with peginterferon
alfa-2b, it is appropriate to consider this therapy as a first-line
treatment for HBeAg -positive chronic hepatitis B,” he said. The
findings of this study are important because chronic hepatitis B
currently affects an estimated 400 million people worldwide, making
it one of the most common infectious diseases and one of the 10
leading causes of death. Chronic hepatitis B is the single most
common cause of liver cirrhosis
and liver cancer.
“Current antiviral therapies, such
as the nucleoside analogues lamivudine (Epivir-HBV)
and adefovir
(Hepsera), do not achieve a durable response and probably are
not effective long -term treatment options due to the inevitable
emergence of drug resistance, Dr. Janssen said.
“Dr. Janssen also explained the importance
of hepatitis B virus genotype as a predictor for response to peginterferon alfa -2b
treatment. “Just like in chronic hepatitis C, the genotype of the hepatitis B virus (HBV) will tell
us what the likelihood of response is. It will become our best tool
towards individualized treatment for patients with HBeAg -positive
chronic hepatitis B,” he said.
[See also Hepatitis
B Virus Genotypes Influence the Response to Antiviral Therapy—Ed]
“The study, organized and sponsored
by the Foundation for Liver Research (SLO), is the first to assess
whether prolonged treatment with peginterferon alfa-2b, alone or
in combination with lamivudine improves sustained treatment response
in patients with HBeAg -positive chronic hepatitis B. HBeAg indicates
that the virus is actively replicating and the infected person is
highly infectious.
“In the study, more patients in the
lamivudine combination group had a response to therapy at the end
of treatment, but the response was not sustained during the follow-up
period. There is growing evidence that only a complete and vigorous
HBV-specific immune response is capable of achieving control and
elimination of the virus, preventing disease progression.
“This suggests that induction of a
host immune response is necessary for sustained response to hepatitis
B treatment, which can only be reached by immunomodulatory therapy,
such as peginterferon alfa-2b,” Janssen said.
Study
Results
“The study was a multicentre, randomized,
double-blind controlled trial conducted at 42 centres in 15 countries
(in Europe, East Asia and North America). The study compared the
efficacy and safety of peginterferon alfa-2b (PEg Intron 100 microgram/week
through 32 weeks; 50 microgram/week 33-52 weeks) with or without
lamivudine (Zeffix) in 307 patients positive for HBeAg (final modified
intent-to-treat analysis n=266).
“Treatment outcomes were assessed at
the end of treatment (EOT) (52 weeks) and again after a 26-week
treatment-free follow-up period (78 weeks).
“The primary endpoint was the percent
of patients who achieved a sustained viral response (SVR) (undetectable levels of serum
HBeAg) at the end of follow-up. Secondary endpoints were
the reduction of HBV DNA levels below 200,000 copies/ml or below
the level of detection (400 copies/ml);
ALT
Normalization and HBsAg Response
“SVR rates were comparable between
the peginterferon alfa-2b monotherapy and combination therapy groups,
36% and 35%, respectively.
“HBV DNA levels at the end of follow-up
were suppressed to below 200,000 copies/ml in 32% of patients in
the combination therapy arm and 27% of patients in the monotherapy
arm. Similarly, there was no difference at the end of followup in
undetectable levels of HBV DNA, 9% and 7%, respectively; ALT normalization,
35% and 32%, respectively; or in HBsAg loss, 7% in both groups.
“Importantly, there was a significant
difference in sustained response rate according to HBV genotype (p=0.01), with HBV genotypes
A (47%) and B (44%) more responsive to therapy than genotypes C
(28%) and D (25%).
“There was no difference in HBeAg loss
according to HBV genotype between the two treatment groups.
Safety
and Tolerability
“Safety and tolerability were similar
for patients treated with peginterferon alfa-2b alone and those treated with lamivudine combination
therapy. The side effect profile of peginterferon alfa-2b was similar to that seen with
standard interferons and there were no new side effects that could be attributable to peginterferon
alfa-2b.
“Overall, the incidence and severity
of adverse events were comparable between the treatment groups.
Common side effects included flu-like symptoms, headache, fatigue
and local reaction at the injection site. There were serious adverse
events in 12% of patients that were reversible after treatment stopped.
“At the end of treatment, 91% of patients
remained on treatment and 69% remained on full-dose treatment.
Source
Erasmus Medical Center, Rotterdam,
The Hague
Reference
1. Pegylated interferon alfa-2b
alone or in combination with lamivudine for HBeAg-positive chronic hepatitis B: a randomised trial;
Harry L.A. Janssen, Monika van Zonneveld, Hakan Senturk, Stefan Zeuzem, Ulus S. Akarca,
Yilmaz Cakaloglu, Christopher Simon, Thomas M.K. So, Guido Gerken,
Robert A. de Man, Hubert G.M. Niesters, Pieter Zondervan, Bettina
Hansen, Solko W. Schalm (for the HBV 99 -01 Study Group). The
Lancet 365:123-129. January 8, 2005.
Additional HIVandHepatitis.com Articles:
- Articles on HBV
Experimental PEG-Intron - Monotherapy
- Articles on HBV
Experimental PEG-Intron plus Epivir-HBV - Combination
Link to Index to All Hepatitis B Articles
- A to Z
|
