HIV Infections Clinical Trial
Official title:
Antiviral Activity of Peg-IFN-Alpha-2A in Chronic HIV-1 Infection
The objective of the study is to compare two different doses of Peg-INF-α-2A (90 or 180 ug/wk) for their ability to maintain viral control when initiated 5 weeks before ART (antiretroviral therapy) interruption in HIV positive, ART-suppressed subjects (viral load <50 copies/ml) as determined by observing the percentages of viral load measurements <400 copies/ml between the two arms over a 24-week period, corresponding to the Pegasys monotherapy period (exclusive of dual ART/Pegasys 5-week period). Primary analysis will be an "intent to treat" analysis and will address the hypothesis that two different doses of Peg-INF-α-2A (90 and 180 ug/week) will be similarly effective at inhibiting viral replication.
The high toxicity of current Anti-Retroviral Therapy (ART) regimens has driven a number of
studies investigating therapeutic approaches aimed at reducing drug exposure while
maintaining the beneficial effects of immune reconstitution. Preliminary observations in
HCV/HIV co-infected individuals already support an antiviral effect by Pegylated
Interferon-Alpha-2A (Peg-IFN-Alpha-2A:Pegasys®) on HIV-1 replication; however, the ability
of Peg-IFN-Alpha-2A (as a single agent) to maintain long-term suppression of HIV-1
replication in patients who interrupt ART after having achieved immune reconstitution
remains undetermined. The rationale for addressing two doses of Peg-IFN-Alpha-2A (180 and 90
ug/week) is based on the antiviral activity reported with both doses and the lower incidence
of adverse events associated with doses lower than that approved for HCV therapy (90 versus
180ug/week).
The long-range goal of this proposal is to determine if Peg-IFN-Alpha-2A monotherapy can
sustain HIV-1 suppression in the absence of ART in infected individuals. Our short-range
goal is to determine the safety, viral suppressive potential and immune correlates of
Peg-IFN-Alpha-2A administered upon the cessation of suppressive ART.
Based on the current literature and our preliminary studies, we hypothesize that weekly
doses of 90 or 180 ug/wk of Peg-IFN-Alpha-2A administered to pharmacologically-suppressed
HIV-infected individuals in the course of antiretroviral therapy (ART) discontinuation will
result in equivalent frequency of viral control, with the lower dose resulting in measurably
lower rate and intensity of therapy-related adverse events (AE).
We propose to compare two different doses of Peg-IFN-Alpha-2A (90 or 180 ug/wk) as a
simplification step to ART, for their ability to maintain viral load suppression when
initiated 5 weeks before ART interruption in HIV-infected, ART-suppressed patients (VL<50
copies/ml). Briefly, control will be determined by the the percentages of viral load
measurements <400 copies/ml between the two arms over a period of 24 weeks, corresponding to
the Pegasys monotherapy period (exclusive of dual ART/Pegasys 5-week period). A threshold of
400 is used based on the known potential for blipping on ART between 50 and 400 copies/ml
with no clinical consequence to sustained suppression thereafter (JAMA 2005, 293:817-829).
Primary analysis will be an "intent to treat" analysis and will address the hypothesis that
two different doses of Peg-IFN-Alpha-2A (90 and 180 ug/week) will be similarly effective at
inhibiting viral replication.
The secondary objectives of the research are:
1. To prospectively evaluate dose-dependent, treatment-associated toxicity, safety and
tolerability of 29 weekly doses of Peg-IFN-Alpha-2A at 180 ug or 90 ug/week (in
association with ART for the initial 5 weeks, followed by 24 weeks of Peg-IFN-Alpha-2A
in the absence of ART).
2. To determine innate immunity outcomes correlated to Peg-IFN-Alpha-2A dose and antiviral
activity by monitoring Natural Killer (NK) and Dendritic cell (DC) subsets changes and
the ability to maintain innate immune function (DC secretory responses, NK antiviral
cytotoxic responses)
3. To determine adaptive immunity outcomes correlated to Peg-IFN-Alpha-2A dose and
antiviral activity by monitoring T-cell subsets changes and the ability to maintain
cell-mediated proliferative and cytokine responses against recall antigens (anti-HIV-1
gag p55).
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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