HIV Infections Clinical Trial
Official title:
Phase II/III Study Evaluating the Effect of IL-2 on Preservation of the CD4 T-Lymphocytes After Interruption of Anti-Retroviral TX in HIV Infected Patients With CD4 T-Lymphocyte Count Greater Than 500 Cells/mm(3) Who Have Received Anti-Retroviral TX
This study will examine whether interleukin-2 (IL-2) given before the interruption of
antiretroviral (ARV) treatment could significantly extend the period of time that a patient
is temporarily not taking ARV treatment and also preserve CD4 counts above 350 cells per
microliter. There will be an evaluation of the toxicity, or extremely harmful effects, of
ARV, and the effect on quality of life.
The use of ARV medications has greatly improved the condition and mortality of HIV-infected
patients. But when used long term, those medications have been associated with great
toxicities and medication fatigue. As a result, patients may not adhere to ARV use, and
resistance to viruses may grow. The CD4 molecule is on the surface of helper T-lymphocytes,
or T-helper cells. It serves as the primary receptor for HIV-1 and HIV-2, allowing the virus
to gain entry into its host. The CD4 count increases immediately in response to ARV, giving
an estimate of the state of a patient's immune system. Thus, it is a strong marker of the
immediate risk of an opportunistic infection, one that takes advantage of a person's
weakened immune system. IL-2 is a molecule naturally produced by activated T cells. In
patients with HIV, IL-2 treatment can increase CD4 counts but the clinical importance of
this increase is not clear. This study will compare the decline in CD4 count, when ARV is
interrupted, in two random groups of participants: (1) those who will receive three cycles
of IL-2 (one every 8 weeks) in combination with ARV therapy for the first 24 weeks of the
study before stopping ARV and (2) those who will receive ARV therapy without IL-2 for 24
weeks before stopping ARV.
Patients 18 years of age or older who have HIV-1 infection and who have been on ARV therapy
for at least 1 year, and who currently have a CD4 count 500 cells per microliter or higher
and never had a CD4 count of less than 200 cells per microliter and a viral load less than
the limit of detection, may be eligible for this study.
Participants will undergo the following procedures and tests:
- Physical examination.
- Blood tests to measure blood lipids (fats), sugar, complete blood count including
platelets, and chemistries.
- Assessment of fat distribution.
- Questionnaire about quality of life.
In addition, those participants who are randomly placed in the group receiving IL-2 and ARV
will get an echocardiogram at the beginning of the study and at week 24. They will receive a
starting dose of 6 million units of IL-2 as an injection under the skin twice a day. Each of
the three IL-2 cycles will last 5 days. After the 24-week period, participants in both
groups will stop taking ARV medications if their CD4 count is still equal to or greater than
500 cells per microliter. The study will continue into 120 weeks. Participants will be asked
to continue to visit the clinic every 8 weeks for evaluation of their viral load and CD4
counts. Every 24 weeks, they will be asked to answer a questionnaire about their quality of
life. Blood tests and other measurements will also be done as follow-up.
The use of antiretroviral (ARV) medications has greatly improved morbidity and mortality of
HIV-infected patients but long-term use of these agents has been associated with significant
toxicities and medication fatigue that can lead to problems with adherence and eventual
development of virologic resistance. The spectrum of ARV toxicities is broad including the
development of lipodystrophy syndrome with lipid abnormalities and glucose intolerance or
diabetes, while increasing evidence suggests an increased risk of cardiovascular
complications in ARV-treated HIV-infected individuals. Current PHHS treatment guidelines
recommend deferring ARV treatment initiation in asymptomatic HIV-infected individuals with
CD4 count greater than or equal to 350 cells/micro liter, and treatment initiation after the
CD4 count is less than 350 cells/micro liter. Several patients who started antiretroviral
therapy at higher CD4 counts (based on older treatment initiation guidelines) or have
experienced significant immunologic reconstitution after ARV initiation, elect to interrupt
antiretroviral therapy until their CD4 count reaches the level of current recommendations
for therapy initiation (less than 350 cells/micro liter).
Studies to date suggest that baseline and nadir CD4 count are the best predictors of a
longer duration of treatment interruption that may be more beneficial with respect to
reversal or delay of long-term ARV-associated toxicity and improved quality of life. It is
known that intermittent cycles of IL-2 administration can lead to expansion of the CD4 pool
and prolong survival of CD4 T cells. In this study the hypothesis tested is that IL-2 given
prior to ARV treatment interruption could significantly prolong the period of ARV treatment
interruption with preservation of CD4 counts above 350 cells/micro liter, and that this
prolongation will be beneficial with respect to antiretroviral related toxicity and quality
of life.
The study will have two parts: during the first part (24 weeks) patients will be randomized
1:1 to either receive three cycles or IL-2 with their ARV therapy or ARV therapy alone. In
the second part (week 24 to week 120), all participants will interrupt therapy and restart
when CD4 is less than 350 cells/micro liter. The main comparison will be at week 72, when
the proportion of patients from the two groups who remain off drugs and have a CD4 greater
than 350 cells/micro liter will be compared. At regular intervals (every 24 weeks)
lipodystrophy measurements and quality of life questionnaires will be evaluated.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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