HIV Infections Clinical Trial
Official title:
A Randomized Trial To Evaluate the Impact of Maintaining Steady-State Concentrations of Azidothymidine (AZT) Versus an Intermittent Schedule of AZT Delivery in Children With Symptomatic HIV Infection
| NCT number | NCT00000982 |
| Other study ID # | ACTG 103 |
| Secondary ID | NCI 89 C-102C |
| Status | Completed |
| Phase | Phase 2 |
| First received | November 2, 1999 |
| Last updated | March 11, 2011 |
AMENDED 07/07/93: To evaluate whether continuous infusion AZT will impact neurodevelopmental
deficits associated with HIV infection or alter rate of encephalopathy progression in
children who have failed to improve or shown progression of these deficits despite optimal
AZT therapy.
AMENDED: To assess whether didanosine (ddI) will be better tolerated than AZT administered
by either continuous intravenous delivery or oral administration (ddI arm removed per
amended version).To determine whether ddI will achieve comparable clinical efficacy as the
continuous intravenous route of delivery of AZT, and to assess whether either or both of
these regimens are superior to that achieved with an intermittent AZT dosage schedule. To
determine whether there are differences in patient or parent (guardian) compliance between
the three treatment regimens. Original design: To determine whether the pharmacokinetic
profile (bloodstream levels) of zidovudine (AZT) influences its effectiveness on HIV
infection in children. That is, the study seeks to find out whether there is a difference in
the effect of AZT when given as a continuous intravenous infusion (and, if available, an
oral sustained release dose) compared to an intermittent (not continuous) dose given orally
every 6 hours. The study also plans to determine (1) whether there are differences in the
tolerance and side effects associated with AZT when given on an intermittent schedule as
opposed to a steady-state schedule; (2) the extent of variation from patient to patient in
AZT levels and whether the plasma and cerebrospinal fluid levels of AZT are related to the
degree of therapeutic effectiveness; and (3) whether there are differences in the response
of children who acquired HIV infection perinatally (just before, during, or just after the
time of birth) versus those who acquired HIV infection by transfusion.
One of the most serious effects of HIV disease in children is neuropsychological
deterioration (relating to mental and nervous system functioning). This complication affects
the vast majority of HIV infected children. A previous study of continuous intravenous
administration of AZT in pediatric patients with HIV infection showed consistent and
dramatic improvements of symptoms in all patients that had shown neurodevelopmental deficits
or abnormalities. These improvements were seen within 3 to 4 weeks after AZT treatment was
started. Neurodevelopmental improvements have been sustained on AZT, usually showing steady
improvement which, in some patients, was associated with restoration of pre-HIV intellectual
and neurological function. This study also showed an increase in the IQ scores of children
receiving continuous infusion of AZT who did not have overt clinical evidence of
encephalopathy (disease of the brain). Thus changes in cognitive function may be among the
earliest signs of AIDS encephalopathy and underscores the need to start therapies that will
treat the central nervous system in patients who appear to be clinically intact. A study
comparing continuous infusion to intermittent dosing of AZT showed a significant increase in
IQ scores for those children receiving the continuous dose compared to those treated with
the intermittent schedule. Although a portable infusion pump allows patients to receive
continuous infusion of AZT, a sustained release oral formulation that could provide a
continuous release of AZT into the bloodstream would be highly desirable.
| Status | Completed |
| Enrollment | 75 |
| Est. completion date | |
| Est. primary completion date | September 1996 |
| Accepts healthy volunteers | No |
| Gender | Both |
| Age group | 3 Months to 12 Years |
| Eligibility |
Inclusion Criteria Concurrent Medication: Allowed: - Steroids for children with lymphocytic interstitial pneumonitis (LIP) who are steroid dependent. - Maintenance amphotericin B and antituberculosis chemotherapy. - Immunoglobulin therapy for children who develop at least three serious bacterial infections while receiving zidovudine (AZT) therapy. - Prophylactic therapy for children who have had a previous episode of Pneumocystis carinii pneumonia (PCP) and who are receiving such therapy. AMENDED 07/07/93: Only HIV-related encephalopathy patients eligible (i.e., children with progressive encephalopathy who have received a minimum of 3 months of oral or intermittent AZT or who have failed to improve following 6 months of optimal AZT). ORIGINAL DESIGN: Eligibility criteria used are similar to those being used in the "Multicenter Trial to Evaluate Oral Retrovir in the Treatment of Children with Symptomatic HIV Infection," currently Protocol 88 C-92a. Children are included: - With overt encephalopathy as well as those who may have a subclinical cognitive impairment. - Children must have laboratory evidence of HIV infection as demonstrated by either a positive viral culture (blood or cerebrospinal fluid) or detectable serum P24 antigen or repeatedly positive test for HIV antibody. HIV antibody must be determined by federally licensed ELISA test and confirmed by Western blot. - Children with AIDS or ARC must have at least one of the following laboratory criteria indicative of immunologic abnormality: - Hypergammaglobulinemia (IgG or IgA) defined as immunoglobulin values greater than upper limit of the age-adjusted normal. - Hypogammaglobulinemia (IgG or IgA) defined as immunoglobulin levels less than lower limit of the age-adjusted normal. - Absolute depression in CD4+ cells of 500 cells/mm3 or less. - Decreased helper/suppressor ratio of 1.0 or less. - Depressed in vitro mitogen response to at least one antigen (pokeweed, phytohemagglutinin, concanavalin A, Staphylococcus aureus, tetanus toxoid, Candida). - Parent or guardian available to give written informed consent. Prior Medication: Allowed within 4 weeks of study entry: - Immunoglobulin for thrombocytopenia. Exclusion Criteria Co-existing Condition: Patients with the following are excluded: - Serious bacterial, fungal, or parasitic infections requiring parenteral therapy, at the time of study entry. Concurrent Medication: Excluded: - Clofazimine, ansamycin (or other experimental agents or agents that may modify zidovudine (AZT) toxicity or safety) for active chronic opportunistic infection at time of study entry. - Chronic use of drugs that are metabolized by hepatic glucuronidation (and may alter the metabolism of AZT) (e.g., acetaminophen). - Prophylaxis for Pneumocystis carinii pneumonia (PCP) for children who have not had a previous episode of PCP, oral candidiasis, or otitis media. - Immunoglobulin therapy not specifically allowed. Patients with the following are excluded: - Serious bacterial, fungal, or parasitic infections requiring parenteral therapy, at the time of study entry. - Lymphocytic interstitial pneumonitis (LIP) and no additional AIDS-defining indicator disease as specified in the CDC Surveillance Case Definition for AIDS. Prior Medication: Excluded within 4 weeks of study entry: - Other antiretroviral agents including ribavirin, HPA-23, dideoxycytosine (ddC), soluble CD4, and dideoxyadenosine (ddA) / didanosine (ddI). - Immunomodulating agents including steroids, interferon, isoprinosine, and IL-2 not specifically allowed. - Immunoglobulin not specifically allowed. - Excluded within 2 weeks of study entry: - Any other experimental therapy. - Drugs that cause prolonged neutropenia or significant nephrotoxicity. Prior Treatment: Excluded within 4 weeks of study entry: - Lymphocyte transfusion for immune reconstitution. - Excluded within 3 months of study entry: - Bone marrow transplant. Risk Behavior: Excluded: - Active alcohol or drug abuse. |
Primary Purpose: Treatment
| Country | Name | City | State |
|---|---|---|---|
| United States | Children's Hosp at Albany Med Ctr | Albany | New York |
| United States | Univ of Maryland at Baltimore / Univ Med Ctr | Baltimore | Maryland |
| United States | Natl Cancer Institute / HIV / AIDS Malignancy Branch | Bethesda | Maryland |
| United States | Walter Reed / USUHS / Pediatrics | Bethesda | Maryland |
| United States | Duke Univ Med Ctr | Durham | North Carolina |
| United States | Univ of Florida Med Ctr | Jacksonville | Florida |
| United States | Children's Hosp of Washington DC / Children's Natl Med Ctr | Washington | District of Columbia |
| Lead Sponsor | Collaborator |
|---|---|
| National Institute of Allergy and Infectious Diseases (NIAID) | National Cancer Institute (NCI) |
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