Clinical Drug Experience Knowledgebase

Criteria

Inclusion Criteria:

Weight 6 kg to less than 40 kg at entry

Antiretroviral therapy (ART)-naïve at entry or has been taking a stable ART regimen for at least six consecutive months at entry

Note: For ART-naïve children, receipt of antiretroviral (ARV) prophylaxis prior to diagnosis of HIV infection is permitted. For these children, ascertainment of this criterion may be based on parent or guardian report only, but available medical records should also be reviewed in relation to this criterion.
Note: For ART-experienced children (on a stable ART regimen), dose and formulation changes (e.g., for growth) within the six months prior to entry are permitted. For these children, ascertainment of this criterion must be based on medical records.

For ART-experienced children (on a stable ART regimen), has had a suppressed HIV viral load (HIV-1 RNA less than 200 copies/mL) for at least six consecutive months prior to entry

Note: To fulfill this criterion, at least two documented HIV-1 RNA results less than 200 copies/mL must be available, one based on a specimen collected at least six months prior to entry and one based on a specimen collected within 30 days prior to entry.
Note: Any documented HIV-1 RNA result greater than or equal to 200 copies/mL based on a specimen collected within six months prior to entry is exclusionary (see exclusion criterion below).

At screening, has normal, Grade 1, or Grade 2 laboratory test results for all of the following, based on testing of specimens collected within 30 days prior to entry and grading per the Division of AIDS Table for Grading the Severity of Adult and Pediatric Adverse Events (refer to the study protocol for guidance on severity grading):

Hemoglobin (greater than or equal to 8.5 g/dL or greater than or equal to 5.25 mmol/L)
Absolute neutrophil count (greater than or equal to 600 cells/mm^3 or greater than or equal to 0.600 x 10^9 cells/L)
Platelet count (greater than or equal to 50,000 cells/mm^3 or greater than or equal to 50.00 x 10^9 cells/L)
Estimated glomerular filtration rate (eGFR; bedside Schwartz formula; greater than or equal to 60 ml/min/1.73 m^2)
Alanine transaminase (ALT) (less than 5.0 x ULN)
Aspartate aminotransferase (AST) (less than 5.0 x ULN)
Total bilirubin (less than 2.6 x ULN)
Direct bilirubin (less than or equal to ULN)
Note: Laboratory tests may be repeated during the screening period (i.e., within 30 days prior to entry), with the latest results used for eligibility determination.
Note: For treatment-experienced children on an atazanavir-containing ART regimen, Grade 3 or higher total bilirubin is permitted.
At screening, has a negative test result for hepatitis B surface antigen based on testing of a specimen collected within 30 days prior to entry

Confirmed HIV-1-infection based on documented testing of two samples collected at different time points:

Sample #1 may be tested using any of the following:

Two rapid antibody tests from different manufacturers or based on different principles and epitopes
One enzyme immunoassay OR Western Blot OR immunofluorescence assay OR chemiluminescence assay
One HIV DNA polymerase chain reaction (PCR)*
One quantitative HIV RNA PCR (above the limit of detection of the assay)*
One qualitative HIV RNA PCR*
One HIV total nucleic acid test*

Sample #2 may be tested using any of the following:

Rapid antibody test. If this option is used in combination with two rapid tests for Sample #1, at least one of the three rapid tests must be United States Food and Drug Administration (FDA)-approved, and the third rapid test must be from a third manufacturer or based on a third principle or epitope.
One enzyme immunoassay OR Western Blot OR immunofluorescence assay OR chemiluminescence assay
One HIV DNA PCR*
One quantitative HIV RNA PCR (above the limit of detection of the assay)*
One qualitative HIV RNA PCR*
One HIV total nucleic acid test*
For participants who are less than two years of age, or who are two years of age and older with any exposure to breast milk in the past 28 days, HIV-1 infection must be confirmed using the tests indicated above with an asterisk (*) for Sample #1 and Sample #2.
Whole blood, plasma, or serum samples must be tested. If both samples are tested using antibody tests, at least one of the samples must be tested in a laboratory that operates according to Good Clinical Laboratory Practice guidelines and participates in an appropriate external quality assurance program. If nucleic acid testing is used, at least one test must be performed in a Clinical Laboratory Improvement Amendments (CLIA) certified (for US sites) or Virology Quality Assurance (VQA) certified (for non-US sites) laboratory. For tests performed in other settings, adequate source documentation including the date of specimen collection, date of testing, test performed, and test result must be available. FDA approved testing methods should be used when possible.

HLA-B*5701-negative based on documented testing at any time prior to entry

Note: Documented testing is required even if the potential participant has received ABC prior to study entry.
For females of reproductive potential (defined as having experienced menarche), not pregnant based on testing performed at screening

For females of reproductive potential who are engaging in sexual activity that could lead to pregnancy, willing to use two methods of contraception while receiving study drug, based on participant and parent or guardian report at entry

One of the two methods must be highly effective; highly effective methods include surgical sterilization (i.e., hysterectomy, bilateral oophorectomy, tubal ligation, or salpingectomy) and the following:

Contraceptive intrauterine device or intrauterine system
Subdermal contraceptive implant
Progestogen injections
Combined estrogen and progestogen oral contraceptive pills
Percutaneous contraceptive patch
Contraceptive vaginal ring
The highly effective method must be initiated prior to study entry. The second method should ideally be a barrier method. Male or female condom use is recommended with all other methods of contraception for dual protection against pregnancy and to avoid transmission of HIV and other sexually transmitted infections.
Based on parent or guardian report at entry, child is expected to be available for 48 weeks of follow-up
Parent or legal guardian is willing and able to provide written informed consent for child's study participation and, when applicable per local institutional review board/ethics committee (IRB/EC) policies and procedures, child is willing and able to provide written informed assent for study participation

Exclusion Criteria:

Documented resistance to ABC, DTG, or 3TC

Note: Testing to rule out resistance is not required, and the M184V resistance mutation is not exclusionary.
For ART-experienced children (on a stable ART regimen), documented HIV-1 RNA result greater than or equal to 200 copies/mL based on a specimen collected within six months prior to entry

History of any of the following as determined by the site investigator based on participant/parent/guardian report and available medical records:

Malignancy (ever)
Hypersensitivity reaction to ABC (ever)
Receipt of any prohibited medication (refer to the study protocol for more information) within 30 days prior to study entry
Receipt of systemic interferon or any chronic systemic immunosuppressant medication within 30 days prior to study entry
Note: Systemic corticosteroids (e.g., prednisone or equivalent up to 2 mg/kg) taken for replacement or short course therapy are permitted. Intranasal or inhaled steroid use is also permitted.

Has any of the following as determined by the site investigator based on participant/parent/guardian report and available medical records

Current clinical evidence of pancreatitis
Currently-active tuberculosis (TB) and/or currently receiving rifampicin-containing TB treatment
Currently-active AIDS-defining (WHO Clinical Stage 4) opportunistic infection
Has any documented or suspected clinically significant medical condition or any other condition that, in the opinion of the site investigator, would make participation in the study unsafe, complicate interpretation of study outcome data, or otherwise interfere with achieving the study objectives