Chronic ethanol use in alcoholic beverages by HIV-infected patients affects the therapeutic window of stavudine, lamivudine and nevirapine during the 9-month follow-up period: using chronic alcohol-use biomarkers
Date
2013Author
Bbosa, Godfrey S.
Kyegombe, David B.
Anokbonggo, William W.
Ogwal-Okeng, Jasper
Musoke, David
Odda, John
Lubega, Aloysius
Ntale, Muhammad
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Background: Chronic ethanol use is a global problem
including among HIV-infected patients on stavudine/
lamivudine/nevirapine (d4T/3TC/NVP) regimen. The
study determined the effect of chronic ethanol use on the
therapeutic window of d4T, 3TC and NVP in HIV-infected
patients using alcohol-use biomarkers to screen patients
for chronic ethanol use.
Methods: A case-control study using repeated measures
design with serial measurements was used to quantify
drugs in plasma. The WHO alcohol use disorder identification
test (AUDIT) tool was initially used to screen patients for
chronic alcohol use, and then they were further sorted using
alcohol-use bioamarkers (γ-glutamyl transferase ≥ 55.0 IU;
mean corpuscular volume, ≥ 96 fl, aspartate amino transferase/
alanine aminotransferase ratio ≥ 2.0 value). A total
of 41 patients (26 in the alcohol group and 15 in the control
group) were followed up for 9 months with blood sampling
done at 3-month intervals. Plasma drug concentrations
were quantified using a Shimadzu Class-VP™ HPLC
data system version 6.1. Data was analyzed using SAS 2003
version 9.1 statistical package with repeated measures fixed
model. Means were compared using Student’s t-test.
Results: The mean steady-state plasma drug concentrations
of d4T and 3TC in the alcohol group were lower than
that in the control group during the 9-month period of
follow-up. For 3TC, there was a statistical difference in the
mean steady-state plasma drug concentrations between
the alcohol group and the control group (p ≤ 0.05) in the 6-
and 9-month period of follow-up. For NVP, in both groups
they were within the reference ranges, although the drug
plasma concentrations were higher in the alcohol group
compared to the control group and were statistically significant
(p < 0.05) in 0, 3 and 6 months of follow-up.
Conclusions: Chronic ethanol use by HIV-infected
patients reduced the therapeutic steady-state plasma drug concentrations of d4T and 3TC and increased the NVP
drug concentrations in the HIV-infected patients.
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