Entecavir
(Baraclude) Demonstrates Greater Antiviral Activity than
Adefovir (Hepsera) in Hepatitis B Patients with Decompensated
Liver Disease
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| SUMMARY:
Entecavir
(Baraclude) exhibited greater antiviral activity
against hepatitis B virus (HBV) than adefovir
(Hepsera) in patients with decompensated liver
cirrhosis, and was associated with clinical benefits
including improved survival, according to a study
presented this past weekend at the 60th Annual
Meeting of the American Association for the Study
of Liver Diseases (AASLD)
in Boston. |
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By
Liz Highleyman
Treatment
of chronic hepatitis B in
patients with decompensated liver disease -- characterized
by symptoms such as ascites (abdominal fluid accumulation),
portal vein hypertension, and hepatic encephalopathy -- has
not been extensively studied, but this group has an urgent
need for effective therapy that can inhibit viral replication
and slow further progression of liver damage.
To
explore this issue, an international team of investigators
conducted a randomized, open-label, Phase 3b study (ETV-048)
comparing 1.0 mg/day entecavir
versus 10 mg/day adefovir
in this population.
A
total of 100 participants randomly assigned to the entecavir
arm and 91 assigned to the adefovir arm started treatment.
Most patients (about 75%) were men and the mean age was
about 52 years. About half were Asian and about one-third
were white. Participants could have prior experience with
interferon
alfa or lamivudine
(Epivir-HBV), but no other anti-HBV therapies. About
one-third had lamivudine resistance.
Just
over half the participants were hepatitis B "e"
antigen (HBeAg) positive. The study population had highly
advanced liver disease. The mean ALT level was about 100
U/L. The mean pre-treatment MELD score was about 16.0, and
the mean Child-Pugh-Turcotte (CPT) score was about 8.5 (all
had a score > 7). About 9% had CTP Class A, about
65% had CTP Class B, and about 25% had CTP Class C liver
disease.
Results
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In
the entecavir arm, 80 patients were treated for 24 weeks
and 71 continued through 48 weeks. |
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In
the adefovir arm, 75 patients were treated for 24 weeks
and 62 for 48 weeks. |
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At
Week 24, mean HBV DNA decreased by 4.48 log10 in the
entecavir arm, compared with 3.40 log10 in the adefovir
arm (P < 0.0001). |
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At
Week 48, HBV DNA decreases were 4.66 log10 and 3.90
log10, respectively. |
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At
Week 24, in a non-completer = failure analysis, 49%
of participants in the entecavir arm achieved HBV DNA
< 300 copies/mL,
compared with 16% in the adefovir arm (P < 0.0001). |
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At
Week 48, the corresponding percentages were 57% and
20%, respectively (P < 0.0001). |
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At
Week 24, 59% of entecavir recipients achieved ALT normalization,
compared with 39% in the adefovir arm (P = 0.0193). |
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At
Week 48, the corresponding percentages were 63% and
46%, respectively (P = 0.0425). |
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At
Week 24, no entecavir recipients achieved HBeAg loss
or seroconversion, compared with 14% loss and 12% seroconversion
in the adefovir arm. |
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By
Week 48, 11% of entecavir recipients achieved HBeAg
loss and 6% experienced seroconversion, compared with
18% and 11%, respectively, in the adefovir arm. |
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At
Week 24, 1% of entecavir recipients (1 person) and no
adefovir recipients achieved hepatitis B surface antigen
(HBsAg) loss. |
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By
Week 48, 5% of entecavir recipients, but still no adefovir
recipients, had achieved HBsAg loss. |
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Mean
MELD score fell by 2.0 points at Week 24 and by 2.6
points at Week 48 in the entecavir arm, compared with
0.9 and 1.7, respectively, in the adefovir arm. |
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A
majority of patients in both arms experienced either
improvement or no further worsening of CTP scores (66%
at Week 24 and 61% at Week 48 in the entecavir arm;
71% and 67%, respectively, in the adefovir arm). |
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In
the entecavir arm, 32% of patients at Week 24 and 35%
at Week 48 experienced at least a 2-point decline in
CTP score, compared with 24% and 27%, respectively,
in the adefovir arm. |
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Patients
in the entecavir arm were more likely to survive and
less likely to develop hepatocellular carcinoma (HCC)
through 288 weeks. |
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23%
in the entecavir arm died during follow-up, compared
with 33% in the adefovir arm. |
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12%
and 20%, respectively, developed HCC. |
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Adverse
event rates were high overall, 89% in the entecavir
arm and 97% in the adefovir arm. |
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54%
and 47%, respectively, experienced grade 3-4 adverse
events. |
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1
entecavir recipient developed lactic acidosis (not requiring
treatment) and 3 had low bicarbonate levels (vs 2 in
the adefovir arm). |
"Entecavir
demonstrated superior antiviral activity to adefovir in this
patient population," the researchers concluded. "Entecavir
provided clinical benefit in patients with chronic hepatitis
B infection and decompensated cirrhosis."
"This
study represents an important first step in addressing an
unmet medical need, as this is one of the first comparative
studies to evaluate the safety and efficacy of antiviral
therapy in this difficult-to-treat patient population,"
said ETV-048 study investigator Hugo Cheinquer in a press
release issued by entecavir manufacturer Bristol-Myers Squibb.
"Chronic hepatitis B is a lifelong disease and these
data suggest that treatment with Baraclude may offer chronic
hepatitis B patients with decompensated cirrhosis a treatment
option."
Chang
Gung Memorial Hospital, Chang Gung University College of
Medicine, Taipei, Taiwan; Aristotle University of Thessaloniki,
Thessaloniki, Greece; Universidade Federal Do Rio Grande
Do Sul, Porto Alegre, Brazil; GB Pant Hospital, New Delhi,
India; Siriraj Hospital, Mahidol University, Bangkok, Thailand;
Alice Ho Miu Ling Nethersole Hospital, Hong Kong, China;
University of Calgary, Calgary, Alberta, Canada; Columbia
University Medical Center, Timisoara, Romania; McGuire VA
Medical Center, Richmond, VA; Medical University, Lodz,
Poland; Research and Development, Bristol-Myers Squibb Company,
Wallingford, CT.
11/3/09
Reference
Y
Liaw, M Raptopoulou-Gigi, H Cheinquer, and others. Efficacy
and Safety of Entecavir versus Adefovir in Chronic Hepatitis
B Patients with Evidence of Hepatic Decompensation. 60th
Annual Meeting of the American Association for the Study
of Liver Diseases (AASLD 2009). Boston. October 30-November
1, 2009. Abstract 422.
Other
source
Bristol-Myers
Squibb. Baraclude
(Entecavir) Demonstrated Greater Antiviral Efficacy Compared
to Adefovir in New Study of Chronic Hepatitis B Patients
with Evidence of Decompensated Cirrhosis. Press release.
October 31, 2009.
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