HIV Infections Clinical Trial
Official title:
A Phase II Study of Intermittent Recombinant Human Interleukin-2 (rhIL-2) by Intravenous or Subcutaneous Administration in Subjects With HIV Infection on Highly Active Antiretroviral Therapy (HAART) Compared to HAART Alone
To compare two different routes of intermittently administered rhIL-2 with a highly active
antiretroviral regimen (HAART) to HAART alone. The comparison is based on the following:
proportion of patients achieving at least 50-percent increase in CD4 counts above
prerandomization baseline values after 1 year of rhIL-2 and the rate of change in CD4
counts. To compare the safety and tolerance of these regimens and their effect on quality of
life. To assess the effects of rhIL-2 when combined with HAART on changes in immune cell
phenotypes and function and on HIV viral load and the rate of antiviral drug resistance
development.
The poor responsiveness of late stage HIV-infected patients to rhIL-2 is thought to occur
because of low T cell regenerative capacity and high viral burden. If means were available
to effectively suppress virus replication, the indigenous immune restorative responses of
the host may be further stimulated and enhanced by rhIL-2. The use of protease inhibitors
with nucleoside-analogue combination regimens appears to be most effective in controlling
virus replication. High-dose intermittent rhIL-2 administered either intravenously or
subcutaneously has been shown to be effective in inducing CD4 responses in a number of
studies.
The poor responsiveness of late stage HIV-infected patients to rhIL-2 is thought to occur
because of low T cell regenerative capacity and high viral burden. If means were available
to effectively suppress virus replication, the indigenous immune restorative responses of
the host may be further stimulated and enhanced by rhIL-2. The use of protease inhibitors
with nucleoside-analogue combination regimens appears to be most effective in controlling
virus replication. High-dose intermittent rhIL-2 administered either intravenously or
subcutaneously has been shown to be effective in inducing CD4 responses in a number of
studies.
All patients receive HAART consisting of two nucleoside analogues (at least one of which is
new to the patient) and the protease inhibitor indinavir for 12 weeks. At Week 10, an HIV
RNA is done. Patients with more than 5,000 copies/ml are taken off the study. Patients with
5,000 copies/ml or less continue on the study and are stratified by their antiretroviral
combination, and randomized to one of three treatment arms. Patients on Arm I continue HAART
alone for an additional 72 weeks. Patients on Arm II continue HAART plus intermittent rhIL-2
by continuous intravenous (CIV) administration for an additional 72 weeks (9 courses).
Patients who achieve both at least a 25-percent increase and at least a 100-cell increase in
CD4 count above prerandomization baseline switch to subcutaneously administered rhIL-2 after
3 courses (24 weeks) or 6 courses (48 weeks) of CIV therapy for the remainder of their
treatment course. Patients on Arm III continue HAART plus subcutaneous rhIL-2 for an
additional 72 weeks (9 courses). [AS PER AMENDMENT 10/31/97: When protocol ACTG 928 is
activated, patients randomized on ACTG 328 are stratified based on whether or not they have
registered on ACTG 928.] [AS PER AMENDMENT 10/30/98: For the 4 weeks immediately prior to
randomization, patients must receive continuous HAART therapy. Exceptions may be made by the
protocol chair for short (i.e., less than 48 hours) interruptions of antiretroviral therapy
during this period. Also per this amendment, two substudies have been added: A5033s and
A5046s. Patients who choose to enroll in substudy A5046s must do so at Week 60 of ACTG 328.
However, if the patient is already beyond Week 60 but not beyond Week 84 of ACTG 328 when
A5046s becomes available, he/she is still encouraged to participate in A5046s. For such
patients, ACTG 328 treatment is extended beyond Week 84 until the patient completes 24 weeks
of A5046s.] [AS PER AMENDMENT 4/23/99: Patients who choose to enroll in substudy A5046s must
do so at or after Week 64 of ACTG 328 and no later than Week 104.] [AS PER AMENDMENT
9/16/99: Patients choosing to enroll in A5046s must do so at or after Week 64 and no later
than Week 128.] [AS PER AMENDMENT 1/22/99: A 16-week treatment extension is provided for
patients who have reached Week 84 of ACTG 328 and intend to enroll in either A5051 or A5046s
(which are currently not available).] [AS PER AMENDMENT 4/23/99: Therapy is extended for 24
weeks beyond the original 84 weeks. Study treatment for patients awaiting co-enrollment into
A5046s continues for up to 20 weeks until co-enrollment and then until completion of A5046s
(24 weeks). Study treatment continues for 24 weeks beyond Week 84 for patients who are
awaiting enrollment in A5051 or who have chosen not to participate in A5046s.] [AS PER
AMENDMENT 6/3/99: A 24-week treatment extension has been added for patients who have reached
Week 100 and intend to enroll in A5046s.] [AS PER AMENDMENT 9/16/99: A treatment extension
has been added for up to 44 weeks beyond Week 84 and through completion of A5046s (24 weeks)
for on-study/on-study treatment patients who intend to co-enroll in A5046s. Patients who
intend to enroll in A5051 or A5046s and remain on ACTG 328 study treatment are eligible for
the treatment extension from Week 84 to Week 108. Patients who intend to co-enroll in A5046s
and remain on ACTG 328 study treatment are eligible for the treatment extension from Week
108 to Week 128. All patients who are awaiting co-enrollment in A5046s must continue to
receive their assigned ACTG 328 treatment regimen. Study treatment for ACTG 328 patients
awaiting co-enrollment into A5046s will continue for up to 44 weeks and until completion of
A5046s (24 weeks). Each patient is followed every 8 weeks for the duration of the treatment
extension period to monitor for safety and to collect cells and plasma for storage. No
substudy evaluations are performed during the 24-week extension.]
;
Endpoint Classification: Safety Study, Primary Purpose: Treatment
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