A Study to Test the Safety, Tolerance, and Metabolism of Abacavir (1592U89, ABC) With Standard Zidovudine (ZDV) Therapy in Newborn Infants Born to HIV-1 Infected Women
- Conditions
- HIV Infections
- Registration Number
- NCT00000864
- Brief Summary
The purpose of this study is to determine the safety, tolerance, and metabolism of single-dose and multiple-dose abacavir (ABC) in HIV-exposed infants receiving standard postnatal treatment with zidovudine (ZDV). This study also evaluates the correct dosages of ABC to be used in future studies.
Early aggressive therapy may be the best chance to slow disease progression in infants who may have been infected with HIV by their mothers. Early HIV suppression may significantly reduce viral levels and allow for restoration of the immune system, providing improved control over HIV infection. Therefore, it is important that the safety and tolerance of ABC in combination with ZDV be examined as potential early therapy in newborn and young infants.
- Detailed Description
The rationale for investigation of this agent is to define the safety and pharmacokinetics in young infants to allow for investigation of the efficacy of this agent in combination with ZDV as potential early therapy in newborn and young infants. The rationale for early aggressive therapy is that this may be the best chance to significantly reduce the long-term progression and subsequent impact of HIV-1 infection in vertically infected infants. Early ablation or enhanced suppression of HIV-1 replication may significantly reduce total viral load and may allow maturation, preservation, or reconstruction of immune function at a stage early in infection providing improved control of HIV-1 infection and reduced disease progression.
This study is divided into 3 sections, as follows: Part 1A is a single-dose study in neonates 0 to 72 hours of age. If four of four patients reach the minimal therapeutic level with less than Grade 3 toxicity, the ABC dose is escalated. Part 1B is also a single-dose study in infants 21 to 28 days of age, starting with the dose identified in Part 1A. If four of four patients reach the minimal therapeutic level with less than Grade 3 toxicity, the dose is escalated again. Finally, Part 2 is a multi-dose study to examine a dosing regimen for ABC and ZDV for neonates 0 to 72 hours of age. The dosing regimen for ABC is the dose defined in Part 1A for the first 3 weeks (0 to 3 weeks of age) followed by the dose defined in Part 1B for the second 3 weeks (3 to 6 weeks of age). All patients receive 6 weeks of standard ZDV therapy.
\[AS PER AMENDMENT 9/24/97: This study is divided into sections, as follows: Part 1A is a single-dose study in neonates 0 to 48 hours of age. ABC dose escalations are made until a dose is identified that meets toxicity guidelines and demonstrates a minimal target area under the concentration curve (AUC) of 2,000 ng-hr/ml. Part 1B is a similar single-dose study in infants 3 to 7 days of age with escalation as per part 1A. Part 1C is an identical single-dose study in infants 21 to 28 days of age but starting at the dose identified in Part 1B. Part 2 is a multi-dose study to examine a 6-week dosing regimen for ABC and ZDV for infants 0 to 48 hours of age. The dosing regimen for ABC is defined in Part 1A for the first 48 hours of life, the dose defined in Part 1B for Days 3 through 20 of life, and the dose defined in Part 1C for Days 21 through 42 of life.\] \[AS PER AMENDMENT 7/29/98: Enrollment to Parts 1A and 1B will remain open; Part 1A will enroll a minimum of 4 patients as planned, and Part 1B will enroll 3 additional patients.\]
Recruitment & Eligibility
- Status
- COMPLETED
- Sex
- All
- Target Recruitment
- 60
Not provided
Not provided
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- Not specified
- Primary Outcome Measures
Name Time Method
- Secondary Outcome Measures
Name Time Method
Trial Locations
- Locations (13)
Univ. of Florida Jacksonville NICHD CRS
πΊπΈJacksonville, Florida, United States
Bronx-Lebanon Hosp. IMPAACT CRS
πΊπΈBronx, New York, United States
San Juan City Hosp. PR NICHD CRS
π΅π·San Juan, Puerto Rico
Med. Univ. of South Carolina, Div. of Ped. Infectious Diseases
πΊπΈCharleston, South Carolina, United States
UCSD Maternal, Child, and Adolescent HIV CRS
πΊπΈSan Diego, California, United States
UAB, Dept. of Ped., Div. of Infectious Diseases
πΊπΈBirmingham, Alabama, United States
Emory Univ. School of Medicine, Dept. of Peds., Div. of Infectious Diseases
πΊπΈAtlanta, Georgia, United States
Usc La Nichd Crs
πΊπΈLos Angeles, California, United States
Univ. of Illinois College of Medicine at Chicago, Dept. of Peds.
πΊπΈChicago, Illinois, United States
DUMC Ped. CRS
πΊπΈDurham, North Carolina, United States
UCLA-Los Angeles/Brazil AIDS Consortium (LABAC) CRS
πΊπΈLos Angeles, California, United States
HMS - Children's Hosp. Boston, Div. of Infectious Diseases
πΊπΈBoston, Massachusetts, United States
SUNY Upstate Med. Univ., Dept. of Peds.
πΊπΈSyracuse, New York, United States