Predicting HIV disease progression in children using measures of neuropsychological and neurological functioning. Pediatric AIDS clinical trials 152 study team

Neuropsychological testing and 2 measures of neurological status, cortical atrophy, and motor dysfunction were assessed for their usefulness in predicting human immunodeficiency virus (HIV) disease progression in infants, children, and adolescents who participated in Pediatric AIDS Clinical Trials G...

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Bibliographic Details
Published in:Pediatrics (Evanston) 2000-12, Vol.106 (6), p.E76-E76
Main Authors: Pearson, D A, McGrath, N M, Nozyce, M, Nichols, S L, Raskino, C, Brouwers, P, Lifschitz, M C, Baker, C J, Englund, J A
Format: Article
Language:English
Subjects:
Acquired Immunodeficiency Syndrome - drug therapy
Adolescent
AIDS Dementia Complex - diagnosis
Anti-HIV Agents - therapeutic use
Brain - diagnostic imaging
Brain - growth & development
CD4 Lymphocyte Count
Child
Child, Preschool
Didanosine - therapeutic use
Disease Progression
Double-Blind Method
Drug Therapy, Combination
Female
HIV-1
Humans
Infant
Intelligence Tests
Male
Neurologic Examination
Neuropsychological Tests
Pediatrics
Predictive Value of Tests
Radiography
Regression Analysis
RNA, Viral - analysis
Zidovudine - therapeutic use
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Summary:Neuropsychological testing and 2 measures of neurological status, cortical atrophy, and motor dysfunction were assessed for their usefulness in predicting human immunodeficiency virus (HIV) disease progression in infants, children, and adolescents who participated in Pediatric AIDS Clinical Trials Group Protocol 152 (PACTG 152). A cohort of 722 antiretroviral therapy-naive children with symptomatic HIV infection were assessed at study entry and at later intervals. Assessments included neurodevelopmental testing, neuroradiologic imaging, and neurological examination of motor function. CD4 cell count and plasma RNA viral load also were measured. Children with the lowest neuropsychological functioning (IQ < 70) at baseline had the highest risk for later HIV disease progression (56%), compared with those with borderline/low (IQ = 70-89) functioning (26%), or with average or above (IQ > 90) functioning (18%). This was also true of week 48 neuropsychological functioning. Motor dysfunction (especially reduced muscle mass) at entry also predicted disease progression. Furthermore, motor dysfunction and week 48 neuropsychological functioning provided predictive information beyond that obtainable from surrogate markers of HIV disease status (eg, CD4 count, HIV RNA level). Children with cortical atrophy also were at higher risk for later disease progression, but when CD4 count and RNA viral load were known, cortical atrophy information provided no additional predictive information. Measures of neuropsychological and motor function status provide unique information regarding pediatric HIV disease progression. As such, these findings have important implications for predicting long-term outcomes (eg, longevity) in pediatric patients.
ISSN:0031-4005
1098-4275