No
Significant Association between Nevirapine (Viramune)
and Liver Enzyme Elevation Regardless of Pregnancy Status
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| SUMMARY:
A new study of more than 2000 women published
in the November 27, 2009 issue of AIDS
found no significant link between use of
the NNRTI nevirapine
(Viramune) and liver enzyme elevation.
Nevirapine use was not associated with liver
toxicity in pregnant or non-pregnant women,
but pregnancy itself increased the risk
of liver problems in women with HIV. |
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Antiretroviral
therapy (ART) during pregnancy significantly reduces
the risk of mother-to-child transmission of HIV. Nevirapine
is commonly used for this purpose in resource-limited
settings, though U.S.
treatment guidelines recommend that pregnant women
should received a complete combination ART regimen.
Current
guidelines advise that nevirapine should not be used
as first-line therapy by women with a CD4 count above
250 cells/mm3 or men with more than 400 cells/mm3.
There is some evidence that use of with nevirapine
during pregnancy is associated with an increased risk
of liver toxicity, especially if a woman has a CD4
cell count above 250 cells/mm3 when she starts therapy.
Investigators
therefore conducted a retrospective study to see if
the association between nevirapine and liver toxicity
differed according to pregnancy status. They analyzed
medical records from 2050 HIV positive women: 1229
(60%) pregnant women on ART in 2 multicenter, prospective
cohorts -- the Women and Infants Transmission Study
and the International Maternal Pediatric Adolescent
AIDS Clinical Trials protocol P1025 -- and 821 (40%)
non-pregnant women from the prospective Women's Interagency
HIV Study cohort.
The
pregnant women were significantly younger, less likely
to have viral hepatitis coinfection, and on average
had higher CD4 cell counts, lower viral loads, and
shorter duration of HIV infection than the non-pregnant
group. However, about three-quarters of women in both
groups had CD4 counts above 250 cells/mm3 (recommendations
against using nevirapine for such patients were instituted
in the mid-2000s).
The
researchers looked at 2 outcomes: Any liver enzyme
elevation (grade 1-4), and severe liver enzyme elevation
(grade 3-4). Elevated liver enzymes, including alanine
aminotransferase (ALT) and aspartate aminotransferase
(AST), are a sign of liver inflammation, and may occur
due to drug toxicity, viral hepatitis, or a variety
of other causes.
Results
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Among
the pregnant women, 174 (14.2%) developed any
liver enzyme elevations and 15 (1.2%) developed
severe elevations. |
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Among
non-pregnant women, the corresponding figures
were 75 (9.1%) and 5 (0.6%), respectively. |
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A
similar proportion of nevirapine recipients and
women who never took nevirapine experienced severe
liver enzyme elevations (0.8% vs 1%, respectively). |
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Nevirapine
was not significantly associated with risk of
liver enzyme elevation, regardless of pregnancy
status. |
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However,
pregnancy was associated overall with an increased
risk of both any liver enzyme elevation and severe
elevation. |
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The
association of pregnancy and liver enzyme elevation
was observed regardless of prior history of ART
or nevirapine exposure. |
Based on these findings, the study authors concluded
that there was no significant association between
nevirapine and liver enzyme elevation, regardless
of pregnancy status. They also found that pregnancy
itself increased the risk of liver toxicity in women
with HIV.
Finally, they wrote, "While we support close
monitoring of pregnant women for clinical or laboratory
evidence of hepatotoxicity with any ART regimen, our
results challenge the notion that nevirapine is uniquely
associated with hepatotoxicity during pregnancy."
Other
Articles on Nevirapine Posted on HIV and Hepatitis.com
12/4/09
Reference
DW Ouyang, DE Shapiro, M Lu, and others. Increased
risk of hepatotoxicity in HIV-infected pregnant women
receiving antiretroviral therapy independent of nevirapine
exposure (Abstract). AIDS 23(18): 2425-2430. November
27, 2009.
