Tenofovir
(Viread) Suppresses HBV Viral Load Long-term in HIV/HBV
Coinfected Patients, but Kidney Function May Decline
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| SUMMARY:
HIV/HBV
coinfected individuals treated with agents
that are dually active against both virus experience
rapid suppression of hepatitis
B virus (HBV), and about 15% of those taking
tenofovir plus emtricitabine (the drugs in the
Truvada
coformulation) achieve hepatitis B "e"
antigen (HBeAg) seroconversion, 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. With long-term use, however, some coinfected
patients may develop persistent kidney impairment. |
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By
Liz Highleyman
Some
nucleoside/nucleotide reverse transcriptase inhibitors (NRTIs)
-- including tenofovir
(Viread), lamivudine
(3TC; Epivir), and emtricitabine
(Emtriva) -- are dually active against both HIV and
HBV. Current antiretroviral
therapy (ART) guidelines recommend that HIV/HBV
coinfected patients should include these drugs in their
antiretroviral regimen.
A
team of Austrian researchers performed a retrospective analysis
of clinical and laboratory data from all HIV/HBV coinfected
patients treated at the HIV outpatient clinic at the Medical
University of Vienna between 1998 and 2009.
A
total of 107 patients were included in the analysis. A majority
(78%) were men and the average age was about 40 years. Most
patients (81%) were on highly active combination ART; 62%
used tenofovir, 42% used lamivudine, and 30% used emtricitabine.
The
mean HBV DNA viral load was 4.35 x10(9) IU/mL before ART
initiation. About two-thirds (65%) of participants were
initially HBeAg positive, and HBeAg positive patients had
significantly higher HBV DNA levels than HBeAg negative
patients (6.45 vs 2.12 x 10(9) IU/mL, respectively). The
most common HBV genotypes were A (56%) and D (38%). The
mean FibroScan liver stiffness measurement was 4.7 kPa at
an average of 7 years after HBV diagnosis, indicating absent
to mild liver fibrosis.
Results
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Over
a median observation period of 61 month, 90% of patients
achieved full HBV viral load suppression (< 350 IU/mL). |
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57%
of patients experience HBeAg seroconversion, with a
cumulative annual probability of 12.0%. |
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The
cumulative annual rate of hepatitis B surface antigen
(HBsAg) loss was 6.6% in HBeAg positive patients and
7.9% in HBeAg negative patients. |
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Patients
receiving tenofovir plus emtricitabine had a slightly
higher annual HBeAg seroconversion rate (14.5%) than
those receiving lamivudine (9.2%) or tenofovir (11.4%)
as the sole dually active agent, but the difference
was not statistically significant. |
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Patients
receiving tenofovir plus emtricitabine also had a higher
annual rate of HBsAg loss (10.3%) compared with those
taking only lamivudine (6.0%) or tenofovir (7.9%), but
again this was not a significant difference. |
|
Annual
HBeAg seroconversion rates were similar regardless of
pre-treatment CD4 cell count (11.3% if > 500 cells/mm3;
13.3% if 200-500 cells/mm3; 12.1% if < 200 cells/mm3). |
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Annual
HBsAg loss rates likewise did not differ significantly
according to pre-treatment CD4 count (10.3%, 8.3%, and
9.1%, respectively). |
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12%
of patients had transient aminotransferase (ALT or AST)
elevations after ART initiation. |
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None,
however, experienced serious (grade 3 or 4) liver toxicity. |
Based
on these findings, the researchers concluded that HIV/HBV
coinfected patients treated with dually active combination
ART "show rapid suppression of HBV replication despite
high baseline viremia and low levels of liver stiffness without
significant hepatoxicity."
They
added that ART containing tenofovir plus emtricitabine "leads
to high rates of HBeAg seroconversion (14.5%/year) and HBsAg
loss (10.3%/year) irrespective of CD4 cell counts."
Gastroenterology
& Hepatology, Medical University of Vienna, Vienna,
Austria; Division of Immunodermatology & Infectious
Diseases, Medical University of Vienna, Vienna, Austria.
Tenofovir
Kidney Toxicity
While
data are mixed, some research indicates that tenofovir can
cause kidney function impairment in a small proportion of
HIV patients, especially those with co-existing risk factors.
However, this association has not been extensively studied
in HIV/HBV coinfected individuals.
In
another study presented at the AASLD meeting, Dutch researchers
assessed the long-term efficacy and safety of tenofovir
as a part of ART in a cohort of 102 HIV/HBV coinfected patients
who took the drug for at least 6 months.
About
three-quarters (77%) of participants had detectable HBV
DNA at baseline. Nearly two-thirds (61%) had previously
used lamivudine, and 42% had lamivudine resistance mutations
at baseline.
Patients
were monitored every 6 months, for a median follow-up period
of 56 months. A standard measure of kidney function, estimated
glomerular filtration rate (eGFR), was calculated using
the Modification of Diet in Renal Disease (MDRD) equation,
based on patient sex, age, race, and serum creatinine level.
Kidney impairment was defined as eGFR less than 60 mL/min/1.73
m2.
Results
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Among 66 HBeAg positive patients, the cumulative probability
of achieving virological response over time was: |
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1
year: 41%; |
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2
years: 74%; |
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3
years: 82%; |
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4
years: 86%; |
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5
years: 89%. |
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There
was no significant difference in response rates between
patients with or without lamivudine resistance at baseline. |
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After
5 years on tenofovir, the rate of HBeAg loss reached
40% and the rate of HBsAg loss reached 9%. |
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Among
13 initially HBeAg negative patients, the cumulative
probability of virological response was: |
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1
year: 54%; |
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2
years: 72%; |
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4
years: 100%. |
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8%
of these patients experienced HBsAg loss. |
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23
patients (all HBeAg negative) had undetectable HBV DNA
at baseline. |
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Within
this subgroup, over a median 53 months of follow-up,
all but 1 (96%) maintained virological suppression,
but none experienced HBsAg loss. |
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Overall,
4 of 102 patients (4%) experienced viral breakthrough,
although none showed evidence of tenofovir resistance
mutations. |
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The
mean eGFR at baseline was 105 mL/min, decreasing significantly
to 94 mL/min by the end of follow-up (P < 0.001).
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During
follow-up, 9 patients (9%) developed kidney impairment. |
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In
3 patients, impairment persisted for more than 3 months. |
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3 participants stopped taking tenofovir due to kidney
problems. |
"[Tenofovir] is an effective anti-HBV agent through
5 years of therapy," the investigators concluded. "Nevertheless,
patients should be carefully monitored for development of
renal impairment, as [tenofovir] therapy is associated with
a significant decline in eGFR."
Department
of Gastroenterology & Hepatology, Department of Internal
Medicine-Infectious Diseases, and Department of Virology,
Erasmus MC, University Medical Center, Rotterdam, Netherlands;
Department of Medical Microbiology (CINIMA) and Division
of Infectious Diseases, Tropical Medicine and AIDS, Academic
Medical Center, Amsterdam, Netherlands.
11/3/09
Reference
LM
Kosi, T Reiberger, K Rutter, and others. High rates of HBeAg
seroconversion and HBsAg loss with Tenofovir + Emtricitabine
in patients with HBV-HIV co-infection irrespective of CD4+
cell count. 60th Annual Meeting of the American Association
for the Study of Liver Diseases (AASLD 2009). Boston. October
30-November 1, 2009. Abstract 391
JG
Reijnders, T de Vries-Sluijs, BE Hansen, and others. Five
year tenofovir therapy is associated with maintained virologic
response, but significant decline in renal function in HIV/HBV
coinfected patients. 60th Annual Meeting of the American
Association for the Study of Liver Diseases (AASLD 2009).
Boston. October 30-November 1, 2009. Abstract 425.
