Validation and Calibration of a Computer Simulation Model of Pediatric HIV Infection | Zendy

Andrea Ciaranello | Zendy; Bethany L. Morris | Zendy; Rochelle P. Walensky | Zendy; Milton C. Weinstein | Zendy; Samuel Ayaya | Zendy; Kathleen Doherty | Zendy; Valériane Leroy | Zendy; Taige Hou | Zendy; Sophie Desmonde | Zendy; Zhigang Lu | Zendy; Farzad Noubary | Zendy; Kunjal Patel | Zendy; Lynn Ramírez-Àvila | Zendy; Elena Losina | Zendy; George R. Seage | Zendy; Kenneth A. Freedberg | Zendy

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Validation and Calibration of a Computer Simulation Model of Pediatric HIV Infection

Author(s) -

Andrea Ciaranello,

Bethany L. Morris,

Rochelle P. Walensky,

Milton C. Weinstein,

Samuel Ayaya,

Kathleen Doherty,

Valériane Leroy,

Taige Hou,

Sophie Desmonde,

Zhigang Lu,

Farzad Noubary,

Kunjal Patel,

Lynn Ramírez-Àvila,

Elena Losina,

George R. Seage,

Kenneth A. Freedberg

Publication year - 2013

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0083389

Subject(s) - calibration , human immunodeficiency virus (hiv) , medicine , virology , computational biology , biology , statistics , mathematics

Background Computer simulation models can project long-term patient outcomes and inform health policy. We internally validated and then calibrated a model of HIV disease in children before initiation of antiretroviral therapy to provide a framework against which to compare the impact of pediatric HIV treatment strategies. Methods We developed a patient-level (Monte Carlo) model of HIV progression among untreated children <5 years of age, using the Cost-Effectiveness of Preventing AIDS Complications model framework: the CEPAC-Pediatric model. We populated the model with data on opportunistic infection and mortality risks from the International Epidemiologic Database to Evaluate AIDS (IeDEA), with mean CD4% at birth (42%) and mean CD4% decline (1.4%/month) from the Women and Infants’ Transmission Study (WITS). We internally validated the model by varying WITS-derived CD4% data, comparing the corresponding model-generated survival curves to empirical survival curves from IeDEA, and identifying best-fitting parameter sets as those with a root-mean square error (RMSE) <0.01. We then calibrated the model to other African settings by systematically varying immunologic and HIV mortality-related input parameters. Model-generated survival curves for children aged 0-60 months were compared, again using RMSE, to UNAIDS data from >1,300 untreated, HIV-infected African children.Results In internal validation analyses, model-generated survival curves fit IeDEA data well; modeled and observed survival at 16 months of age were 91.2% and 91.1%, respectively. RMSE varied widely with variations in CD4% parameters; the best fitting parameter set (RMSE = 0.00423) resulted when CD4% was 45% at birth and declined by 6%/month (ages 0-3 months) and 0.3%/month (ages >3 months). In calibration analyses, increases in IeDEA-derived mortality risks were necessary to fit UNAIDS survival data.Conclusions The CEPAC-Pediatric model performed well in internal validation analyses. Increases in modeled mortality risks required to match UNAIDS data highlight the importance of pre-enrollment mortality in many pediatric cohort studies.

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