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Session 143
Poster Abstracts NRTI Toxicities Wednesday, 1:30 - 3:30 pm Hall B |
Background: Didanosine (ddI) plus tenofovir (TDF) is a combination with several potential
advantages (once a day and high genetic barrier), but also pitfalls (unexpected
CD4 drops and increased risk of pancreatitis). Since
several cases of transient insulin-dependent diabetes mellitus were seen in our
clinic in patients on ddI- and
TDF-containing regimens, we explored the rate of this
complication in more detail.
Methods: Retrospective analysis of plasma glucose
levels in patients who completed 12 months follow-up under 3 different triple
HAART regimens including ddI+TDF, TDF, or ddI. Patients under anti-diabetic agents and those whose
baseline glucose level was > 125 mg/dL were
excluded. Weight, age, concomitant ART, and ddI
dosage were assessed. At 12 months without treatment changes, fasting glucose levels were
compared with baseline. A multivariate analysis was performed to evaluate
which variables were associated with glucose elevation.
Results: We included 177 HIV+
patients in the analysis: ddI+TDF (n = 78), TDF (n = 42), and
ddI (n = 57). Mean values
at baseline were balanced between groups: age 39 ± 7 years; 78% male; CD4+ count 507 ± 300 cells/mm3; weight 67 ± 11 kg. There were only significant
differences between groups regarding concomitant proetasae inhibitor (PI) use (13% with ddI+TDF vs 7% and 8% with TDF and
ddI, respectively). At 12 months,
ddI daily dose was 250 mg
and 400 mg in 60% and 40% of ddI+TDF recipients, respectively (ddI dose reduction with concomitant TDF use had not been
advised at that time). At 12 months, hyperglycemia was significantly
more frequent in ddI+TDF recipients (33%) when
compared with patients on TDF or ddI (5% and 10%,
respectively). Multiple linear regression was performed considering variation
of glucose levels at 12 months as dependent variable and treatment with ddI or TDF, weight, age, and PI concomitant use as
independent factors. A lower baseline weight (b –0.35; 95% CI –0.67 to –0.03; p = 0.033) and
use of regimens including ddI+TDF (b 13.05; 95% CI 0.2 to 26; p = 0.047) were independently
associated with higher glucose values.
Conclusions: The risk of hyperglycemia
is increased in patients on ddI+TDF, particularly
among those with lower baseline weight. As high ddI
exposure has been related to endocrine pancreatic dysfunction and diabetes, ddI “overdosing” (related to lower weight and potentiated by TDF use) may be an explanation for our
findings. Our results add a further note of caution to the concomitant use of
TDF and ddI.
Keywords: Hyperglycemia; Didanosine; Tenofovir
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