Acute HIV Infection Clinical Trial
Official title:
Viral Suppression After Analytic Treatment Interruption in Thai Patients Who Initiated Highly Active Antiretroviral Therapy During Acute HIV Infection
This is a Phase 2, two-step, open-label study of the outcome of analytic treatment
interruption (ATI) on patients who started antiretroviral therapy (ART) during Fiebig Stage
I of acute HIV infection (AHI), defined as detectable HIV-RNA without detectable p24 antigen
or HIV IgM. The primary endpoint will be rate of sustained viral suppression, defined as
HIV-1 RNA < 50 cps/ml at 24 weeks after treatment interruption. During ATI subjects will be
monitored closely for safety and will have ART re-initiated if they meet predefined
clinical, virological, or immunological criteria. In step I, there will be 8 subjects who
undergo ATI. An interim analysis for safety will be conducted after 12 weeks. If none of the
subjects maintain viral suppression at 12 weeks then no further subjects will be enrolled
into the study. If at least 1 out of 8 subjects maintains viral suppression at 12 weeks then
an additional 7 subjects will be enrolled in step 2.
At ATI all antiretroviral drugs will be discontinued. Subjects will be monitored with
clinical exam, immunological (CD4), and virological (HIV-RNA) testing at baseline and then
on a fixed schedule for 24 weeks. ART will be re-initiated immediately if subjects meet any
pre-defined clinical, immunological or virological safety endpoints during the monitoring
period.
This is a two step open label study of ATI in patients who initiated ART in the earliest
detectable stage (Fiebig I) of HIV infection. In step I, eight subjects will discontinue ART
for a period of up to 24 weeks. An interim assessment will be conducted after all eight
subjects in step I complete follow-up for 12 weeks. If at least one out of eight subjects
maintains viral suppression (HIV-1 RNA < 50 copies/ml) at 12 weeks, then the study will
proceed to step 2, in which 7 additional subjects (maximum total sample size of 15) will
undergo ATI. The primary endpoint is proportion of subjects who maintain viral suppression
at 24 weeks post ATI. Subjects will be monitored frequently for disease progression using
clinical, immunological and virological criteria. ART will be re-initiated immediately for
any subjects who meet pre-defined criteria for disease progression.
Parent Study Cohort
This is a sub-study of the protocol "Establish and characterize an acute HIV infection
cohort in a high-risk population" (SEARCH 010, RV254, WRAIR 1494) implemented at the Thai
Red Cross AIDS Research Center in Bangkok, Thailand. From April 2009 through February 2014
the cohort had enrolled 150 patients with acute infection and 145 (97%) are still in active
follow-up. All patients in the cohort are offered ART at the time of enrollment through a
separately funded protocol; all 145 subjects (100%) in active follow-up are currently on
ART. The median age (range) of the cohort is 28 (18-57) years and 90% are men who have sex
with men (MSM).
The cohort currently has 50 volunteers who started ART during Fiebig Stage 1, of whom 24
have been on ART for > 24 months and have HIV-1 < 50 copies/ml. Another 13 volunteers have
been on ART 6-24 months with undetectable HIV-1 RNA.
During the period of co-enrollment in this substudy, no additional biological specimens will
be collected as part of the RV254/SEARCH 010 protocol. Data and samples from this substudy
will be shared with the parent protocol.
Criteria to reinitiate ART after ATI
The criteria to restart ART after ATI are designed to protect the subjects from any possible
clinical, immunological, or virological adverse effects in the event that their VL rebounds
while off ART. The viral load (VL) criterion of > 1,000 copies/ml was chosen because
clinical symptoms of HIV infection or significant decline in CD4 count would not be expected
at this low level of viremia. The Fiebig I patients in the SEARCH 010 cohort had a median
(range) HIV-1 RNA of 4.8 (2.8-5.7) log10copies/ml, at a median (range) of 12 (4-40) days
after exposure to HIV, prior to initiation ART and have therefore already been exposed to
high levels of plasma virus during acute infection while maintaining low or no detectable
HIV proviral reservoirs.
In addition, the ANRS Visconti study found that patients who are virologic controllers
(sustained VL < 50 copies/ml) after ATI may initially and transiently have VL above
detection. Of 240 tests performed after treatment interruption in those who were
subsequently virologic controllers or PTC, 2% had VL > 400 copies/ml and 18% had VL between
50 and 400 copies/ml. Therefore, low-level viremia may not always be indicative of viral
rebound and can potentially reverse.
Specific criteria for re-initiation of ART after ATI are:
1. HIV-1 RNA above 1,000 copies/ml on 2 consecutive determinations at least 3 days apart.
OR
2. HIV-1 RNA rise of ≥ 0.5 log10copies/ml per day provided that the last HIV-1 RNA is
above 1000 copies/ml OR
3. A single HIV-1 RNA above 10,000 copies/ml OR
4. CD4+ T-cell counts below 350 cells/mm3 on 2 consecutive determinations at least 2 weeks
apart. OR
5. CD4+ T-cell count decline of > 50% from baseline prior to ATI. OR
6. Clinical progression to CDC Category B or C disease. OR
7. Diagnosis of Acute Retroviral Syndrome. OR
8. Pregnancy OR
9. Subject requests re-initiation of ART.
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