HIV Infection Clinical Trial
Official title:
A Randomized, Controlled Trial of Short Cycle Intermittent Versus Continuous HAART for the Treatment of Chronic HIV Infection
This study will evaluate the effects of intermittent short cycles of HAART (highly active
antiretroviral therapy) for treating HIV infection. HAART is a multi-drug regimen that is
very effective in suppressing HIV and perhaps slowing or halting progression to AIDS.
However, the treatment has significant drawbacks: it cannot completely rid the body of
virus; long-term therapy carries a risk of toxicity (harmful side effects); and the regimen
is difficult to comply with because many pills and capsules must be taken daily. When
patients stop taking HAART, their HIV levels climb again. This study will see if giving
HAART in short cycles of 7 days on, 7 days off, can keep viral levels low while maintaining
CD4+ T cell counts.
HIV-infected people age 18 or older who are receiving HAART and have a viral load of less
than 50 copies/ml and a CD4+ T cell count of at least 175 cells/mm3 may be eligible for this
study. Candidates will be screened with a medical history and physical examination, blood
and urine tests, and possibly a chest X-ray and electrocardiogram. Women of childbearing
potential will have a pregnancy test.
Participants will be randomly assigned to either continue their current medication regimen
or to take HAART in intermittent cycles of 7 days off, 7 days on. Patients will continue
treatment for 72 weeks or until viral levels increase or CD4+ T cell counts decline to a
level of concern.
Upon entering the study, patients will have blood tests to monitor the amount of virus in
the blood, CD4+ T cell count, viral resistance to HAART medications, side effects of the
drug, and immune response to HIV in the test tube. They will have clinic visits for a
history, physical examination and blood draws every month for 12 months. At that time,
depending on T cell counts and viral load, the number of visits may be reduced, but never
less frequently than every other month.
Patients will also undergo leukapheresis-a procedure for collecting quantities of white
blood cells-every 3 to 4 months while on the study. For this procedure, whole blood is
collected through a needle in an arm vein (similar to donating blood). The blood is
circulated through a cell separator where the white cells are removed, and the rest of the
blood (plasma, red cells and platelets) is returned through the same needle or through a
second one in the other arm. The collected white cells are used for special studies on the
level and function of T cells and to detect hidden virus.
| Status | Completed |
| Enrollment | 90 |
| Est. completion date | January 2005 |
| Est. primary completion date | |
| Accepts healthy volunteers | No |
| Gender | Both |
| Age group | N/A and older |
| Eligibility |
INCLUSION CRITERIA: Documentation of HIV-1 infection by licensed ELISA test kit and confirmed by a second method (e.g. Western Blot). Absolute CD4+ T-cell count of greater than or equal to 175/mm(3) within 30 days before randomization (For patients who are status post-splenectomy, also CD4+ T-cell greater than 20%). If the CD4+ T cell count is less than or equal to 200 cells/mm(3), the patient must be receiving PCP prophylaxis. Receiving at least 3-drug HAART with at least 1viral load test less than 500 copies/ml and within at least 6 months screening. Patients must be receiving an NNRTI or a PI at enrollment. A viral load of less than 50 copies/ml prior to enrollment. Age at least 18 years. For women of childbearing potential, a negative pregnancy test (serum or urine) is required within 14 days prior to randomization. Laboratory values (within 30 days prior to randomization): 1. AST no more than 5 X the upper limit of normal (ULN). 2. Total or direct bilirubin no more than 2 X ULN unless there is a pattern consistent with Gilbert's syndrome or the patient is receiving indinavir. 3. Creatinine no more than 2.0 mg/dL. 4. Platelet count at least 50,000/microliter. EXCLUSION CRITERIA: Concurrent malignancy, or any other disease state, requiring cytotoxic chemotherapy. Symptomatic for significant HIV-related illnesses, such as opportunistic infections and malignancies other than mucocutaneous Kaposi's sarcoma. A history of AIDS defining opportunistic infections other than mucocutaneous candida. Use experimental antiretrovirals less than or equal to 6 months prior to enrollment. An exception may be made for hydroxyurea according to the judgment of the Principal Investigator. Patients receiving IL-2 will be eligible, and will be required to cycle during an on-HAART period if they are randomized to the intermittent arm. Pregnant or breastfeeding. Significant cardiac, pulmonary, kidney, rheumatologic, gastrointestinal, or CNS disease as detectable on routine history, physical examination, or screening laboratory studies. Psychiatric illness that, in the opinion of the PI, might interfere with study compliance. Active substance abuse or history of prior substance abuse that may interfere with protocol compliance or compromise patient safety. Refusal to practice safe sex or use precautions against pregnancy (effective birth control with barrier contraceptives or abstinence). Known history or laboratory evidence of chronic hepatitis B infection including surface antigen positivity. Receiving salvage HAART, i.e. no evidence of clinical resistance to licensed anti-retrovirals. Patients receiving nevirapine, abacavir amd single protease inhibitor regimes at the time of enrollment. Patients receiving these medications may switch to other approved agents, and if the plasma viremia remains less than 50 copies/ml at least 30 days later, they would be eligible for enrollment. Patients on the continuous arm may receive nevirapine or abacavir regimens while participating in that arm. |
Endpoint Classification: Efficacy Study, Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| United States | National Institute of Allergy and Infectious Diseases (NIAID) | Bethesda | Maryland |
| Lead Sponsor | Collaborator |
|---|---|
| National Institute of Allergy and Infectious Diseases (NIAID) |
United States,
García F, Plana M, Vidal C, Cruceta A, O'Brien WA, Pantaleo G, Pumarola T, Gallart T, Miró JM, Gatell JM. Dynamics of viral load rebound and immunological changes after stopping effective antiretroviral therapy. AIDS. 1999 Jul 30;13(11):F79-86. — View Citation
Neumann AU, Tubiana R, Calvez V, Robert C, Li TS, Agut H, Autran B, Katlama C. HIV-1 rebound during interruption of highly active antiretroviral therapy has no deleterious effect on reinitiated treatment. Comet Study Group. AIDS. 1999 Apr 16;13(6):677-83. — View Citation
Zhang L, Ramratnam B, Tenner-Racz K, He Y, Vesanen M, Lewin S, Talal A, Racz P, Perelson AS, Korber BT, Markowitz M, Ho DD. Quantifying residual HIV-1 replication in patients receiving combination antiretroviral therapy. N Engl J Med. 1999 May 27;340(21):1605-13. — View Citation
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