HIV Infections Clinical Trial
Official title:
A Randomised, Controlled, Open-Label, 48-Week, Study To Asses Differences in Changes In Plasma Lipid Profile Between Patients On Saquinavir/Ritonavir Or Atazanavir/Ritonavir In Combination With Tenofovir Disoproxil Fumarate And Emtricitabine As A First-line Regimen.
The purpose of this study is to assess differences in changes in plasma lipids between patients on saquinavir/ritonavir or atazanavir/ritonavir in combination with tenofovir disoproxil fumarate and emtricitabine as a first-line regimen in patients previously naive for antiretroviral therapy. This study is an extension from the SSAR 2004/0002 which randomised patients over the same treatment arms.
The main objective of the study is to measure changes in blood lipids during 48 weeks of
treatment with saquinavir (SQV) / ritonavir (RTV) or atazanavir (ATV) / RTV, in combination
with tenofovir (TDF) / emtricitabine (FTC). All of these medications are commonly used for
the treatment of HIV-1 infection. When the initial anti-HIV therapy is selected, several
important issues are considered such as the effectiveness, the possible long- and/or
short-term side effects, the frequency of medication intake and the amount of pills that
needs to be taken.
There is currently some concern about the long-term metabolic side effects of existing
treatment regimens. Metabolic disorders, such as elevated blood lipids (including
cholesterol) and a decreased sensitivity for insulin, which increases the chance of
diabetes, pose an increased risk of cardiovascular disease. A large cohort study (the D:A:D
study), executed worldwide, including in Dutch hospitals, has actually shown that the use of
HIV combination therapy coincides with an increased risk of developing cardiovascular
disease. A certain category of HIV inhibitors, the protease inhibitors, are particularly
associated with elevated blood lipids. Results from the afore-mentioned worldwide study have
recently indicated that in particular the use of protease inhibitors increases the risk of
cardiovascular disease, which can to an important extent be explained by a change in the
blood lipids caused by these medications. There are however some protease inhibitors, such
as the recently developed drug atazanavir (ATV) and the protease inhibitor saquinavir (SQV)
that has already been available for several years, which show no to only a little effect on
blood lipids. SQV had the disadvantage of having to be dosed twice-daily, with many capsules
(10-12 in total per day). Now that a new SQV tablet has been developed, the number of
capsules to be taken per day has decreased dramatically (to only 4 in total per day) and
moreover it has become possible in actual practice to take these capsules once per day. It
is advisable, for both SQV and ATV, to combine the medication with one capsule of ritonavir
(RTV), another protease inhibitor. This ensures that a reliable and effective level of SQV
or ATV will be reached in the blood. RTV is associated with elevated blood lipids, but this
effect is very limited in the low dosage that is used in combination with ATV or SQV. And as
both SQV and ATV are combined with an equal amount of RTV, it is expected that their
favorable effect on the blood lipids will be the same. For the same reason, the risk of
cardiovascular disease is expected to be equally limited with the use of either of these two
regimens.
In addition to long-term effects on the blood lipids, which poses a risk of cardiovascular
disease, a disturbed fat distribution (lipodystrophy) is another frequently occurring
complication in the treatment of HIV-1 infection. This disturbed fat distribution is
associated with subcutaneous fat loss in some body parts (particularly the face, arms and
legs, and buttocks) and with fat accumulation in other body parts (such as the abdomen, the
back of the neck and female breasts). Subcutaneous fat loss is mainly associated with
thymidine-containing nucleoside analogues like zidovudine (AZT) and stavudine (d4T).
Previous studies in patients receiving antiretroviral treatment for the first time have
shown that a combination of TDF / lamivudine (3TC) (the latter drug closely resembles FTC)
does not lead to loss of subcutaneous fat (lipoatrophy), as opposed to the combination d4T /
3TC or AZT / 3TC. The cause of fat accumulation is however less clear, but often coincides
with changes in blood lipids. The chance of the occurrence of fat accumulation could thus
depend on the extent to which an HIV combination therapy coincides with an elevation of
blood lipids.
As it is now becoming clear that there are initial therapies involving less risk of
long-term side effects, it is important to develop therapy schedules that are safe with
regard to these aspects. According to what has been described before, a combination of
either ATV / RTV or SQV / RTV, administered together with TDF and FTC to prevent fat loss,
would be a good initial regimen, as these combinations have little to no effect on the blood
lipids and may therefore decrease the chance of fat accumulation. A big advantage of the use
of combination therapy with protease inhibitors in combination with a low dose of RTV is
that it largely diminishes the chance of the development of resistance to HIV protease
inhibitors, even if the virus becomes detectable in the blood again after initial
suppression - as opposed to the most commonly used alternative initial therapy in which
non-nucleoside reverse transcriptase inhibitors are used instead of protease inhibitors.
With the use of these drugs, the risk of resistance is much greater. It is therefore
essential to better examine these protease-inhibitor-containing regimens, which are expected
to have the advantage of producing a minimal effect on the lipid and sugar metabolism as
well as a limited chance of resistance development.
In the BASIC study we want to show that SQV / RTV is comparable to ATV / RTV with regard to
the effect on blood lipids. We will also look in detail at the effects on fat loss and fat
accumulation, as well as on sugar metabolism and insulin sensitivity, in the hope that only
very limited changes in these areas will be demonstrated.
One study in which patients were given their first antiretroviral treatment demonstrated a
slight decrease in bone density (a form of bone loss) in the first year of treatment with
TDF and FTC (which closely resembles 3TC). This did however not cause any clinical problems.
It was very reassuring to see that a complete recovery of the bone density was again seen
after this first year. Nevertheless we want to collect more data about the possible effects
on the bone metabolism and for this reason we will perform two bone density assessments
during this study. Finally, there are indications that the renal function in patients who
are treated with TDF may become slightly disturbed. It is as yet not clear which method can
most accurately estimate and detect these slight changes in renal function. For this reason,
we plan to compare a number of different methods to estimate renal function as part of this
study. For this purpose a number of additional relevant measurements will be obtained using
the blood samples which are already being collected as part of the study anyway.
The main purpose of the study is to measure changes in the blood lipids and to compare these
between patients who start with either an SQV / RTV-containing regimen or an ATV /
RTV-containing regimen. In addition, the changes in fat distribution, sugar metabolism and
insulin sensitivity will be compared between these groups. Possible changes in bone density
and renal function will also be examined. Furthermore, the virologic effectiveness and
overall safety of the two treatments will be evaluated and compared.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
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