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Enhanced
Saquinavir Exposure in HIV Patients with Diarrhea and/or Wasting
Syndrome
The
protease inhibitor Invirase
(saquinavir) was administered to 100 human immunodeficiency virus
type 1 (HIV-1)-infected patients as a single 600-mg oral dose (hard
gelatin capsules) with a standard breakfast, including 200 ml of
grapefruit juice, during an open-label trial conducted in France
to assess whether diarrhea and/or wasting syndrome has consequences
on its pharmacokinetics.
Three
groups of patients were enrolled: group 1, asymptomatic patients
(n = 30); group 2, AIDS symptomatic patients without body weight
loss or diarrhea (n = 37); and group 3, AIDS symptomatic patients
with severe body weight loss and/or diarrhea (n = 33). Clinical
and biological data (covariates) were collected.
A
population approach was performed with three blood samples per patient
to estimate the mean population pharmacokinetic parameters (clearance
[CL]/oral bioavailability [F], V/F, k(a), and lag time) and the
derived ones (k(el), C(max), T(max), and area under the curve [AUC]).
The relationships between groups, exposure (i.e., estimated individual
post hoc AUCs), and covariates were explored by using multiple linear
regressions.
Results
A
significant increase in median AUCs (165, 349, and 705 ng. h. ml(-1)
for groups 1, 2, and 3, respectively [P < 0.0001]) was observed.
The enhancement in saquinavir exposure could be due to the destruction
of the transporters in enterocytes and/or to the enlargement of
their tight junctions, allowing a paracellular crossing of saquinavir
as the illness spreads.
Because
of grapefruit juice intake by every patient, no implication of CYP3A4
could be assessed. These results strongly suggest that, despite
its low intrinsic oral bioavailability, saquinavir can be considered
as a relevant treatment for HIV-1-infected patients with diarrhea
and/or wasting syndrome. This must be evaluated in a long-term period.
02/04/04
Reference
H
Trout and others. Enhanced Saquinavir Exposure in Human Immunodeficiency
Virus Type 1-Infected Patients with Diarrhea and/or Wasting Syndrome.
Antimicrobial
Agents and Chemotherapy 48(2): 538-545. February 2004.
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