TY - JOUR
T1 - Comparing longitudinal CD4 responses to cART among non-perinatally HIV-infected youth versus adults
T2 - Results from the HIVRN Cohort
AU - HIV Research Network
AU - Agwu, Allison L.
AU - Fleishman, John A.
AU - Mahiane, Guy
AU - Nonyane, Bareng Aletta Sanny
AU - Althoff, Keri N.
AU - Yehia, Baligh R.
AU - Berry, Stephen A.
AU - Rutstein, Richard
AU - Nijhawan, Ank
AU - Mathews, W. Christopher
AU - Aberg, Judith A.
AU - Keruly, Jeanne C.
AU - Moore, Richard D.
AU - Gebo, Kelly A.
AU - Edelstein, Howard
AU - Corales, Roberto
AU - Jacobson, Jeffrey
AU - Allen, Sara
AU - Beil, Robert
AU - Hanau, Lawrence
AU - Korthuis, P. Todd
AU - Akbar, Muhammad
AU - Gaur, Aditya
AU - Sharp, Victoria
AU - Arpadi, Stephen
AU - Somboonwit, Charurut
AU - Cohn, Jonathan
AU - Hellinger, Fred
AU - Fraser, Irene
AU - Mills, Robert
AU - Malitz, Faye
AU - Voss, Cindy
PY - 2017/2
Y1 - 2017/2
N2 - Background Youth have residual thymic tissue and potentially greater capacity for immune reconstitution than adults after initiation of combination antiretroviral therapy (cART). However, youth face behavioral and psychosocial challenges that may make them more likely than adults to delay ART initiation and less likely to attain similar CD4 outcomes after initiating cART. This study compared CD4 outcomes over time following cART initiation between ART-naïve non-perinatally HIV-infected (nPHIV) youth (13-24 years-old) and adults (≥25-44 yearsold). Methods Retrospective analysis of ART-na?ve nPHIV individuals 13-44 years-old, who initiated their first cART between 2008 and 2011 at clinical sites in the HIV Research Network. A linear mixed model was used to assess the association between CD4 levels after cART initiation and age (13-24, 25-34, 35-44 years), accounting for random variation within participants and between sites, and adjusting for key variables including gender, race/ethnicity, viral load, gaps in care (defined as > 365 days between CD4 tests), and CD4 levels prior to cART initiation (baseline CD4). Results Among 2,595 individuals (435 youth; 2,160 adults), the median follow-up after cART initiation was 179 weeks (IQR 92-249). Baseline CD4 was higher for youth (320 cells/mm3) than for ages 25-34 (293) or 35-44 (258). At 239 weeks after cART initiation, median unadjusted CD4 was higher for youth than adults (576 vs. 539 and 476 cells/mm3, respectively), but this difference was not significant when baseline CD4 was controlled. Compared to those with baseline CD4 ≤200 cells/mm3, individuals with baseline CD4 of 201-500 and >500 cells/ mm3 had greater predicted CD4 levels: 390, 607, and 831, respectively. Additionally, having no gaps in care and higher viral load were associated with better CD4 outcomes. Conclusions Despite having residual thymic tissue, youth attain similar, not superior, CD4 gains as adults. Early ART initiation with minimal delay is as essential to optimizing outcomes for youth as it is for their adult counterparts.
AB - Background Youth have residual thymic tissue and potentially greater capacity for immune reconstitution than adults after initiation of combination antiretroviral therapy (cART). However, youth face behavioral and psychosocial challenges that may make them more likely than adults to delay ART initiation and less likely to attain similar CD4 outcomes after initiating cART. This study compared CD4 outcomes over time following cART initiation between ART-naïve non-perinatally HIV-infected (nPHIV) youth (13-24 years-old) and adults (≥25-44 yearsold). Methods Retrospective analysis of ART-na?ve nPHIV individuals 13-44 years-old, who initiated their first cART between 2008 and 2011 at clinical sites in the HIV Research Network. A linear mixed model was used to assess the association between CD4 levels after cART initiation and age (13-24, 25-34, 35-44 years), accounting for random variation within participants and between sites, and adjusting for key variables including gender, race/ethnicity, viral load, gaps in care (defined as > 365 days between CD4 tests), and CD4 levels prior to cART initiation (baseline CD4). Results Among 2,595 individuals (435 youth; 2,160 adults), the median follow-up after cART initiation was 179 weeks (IQR 92-249). Baseline CD4 was higher for youth (320 cells/mm3) than for ages 25-34 (293) or 35-44 (258). At 239 weeks after cART initiation, median unadjusted CD4 was higher for youth than adults (576 vs. 539 and 476 cells/mm3, respectively), but this difference was not significant when baseline CD4 was controlled. Compared to those with baseline CD4 ≤200 cells/mm3, individuals with baseline CD4 of 201-500 and >500 cells/ mm3 had greater predicted CD4 levels: 390, 607, and 831, respectively. Additionally, having no gaps in care and higher viral load were associated with better CD4 outcomes. Conclusions Despite having residual thymic tissue, youth attain similar, not superior, CD4 gains as adults. Early ART initiation with minimal delay is as essential to optimizing outcomes for youth as it is for their adult counterparts.
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U2 - 10.1371/journal.pone.0171125
DO - 10.1371/journal.pone.0171125
M3 - Article
C2 - 28182675
AN - SCOPUS:85012072436
SN - 1932-6203
VL - 12
JO - PloS one
JF - PloS one
IS - 2
M1 - e0171125
ER -