4.7 Article

Early antiretroviral therapy initiation effect on metabolic profile in vertically HIV-1-infected children

Journal

JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY
Volume 76, Issue 11, Pages 2993-3001

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/jac/dkab277

Keywords

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Funding

  1. Fondo de Investigacion Sanitaria-ISCIII-FEDER (European Regional Development Fund/European Social Fund
  2. 'A way to make Europe'/'Investing in your future') [PI16/00503, PI19/01337, PI19/01638, PI20/00326]
  3. Programa de Suport als Grups de Recerca AGAUR [2017SGR948]
  4. Spanish AIDS Research Network-ISCIII-FEDER (Spain) [RD16/0025/0006, RD16/0025/0019]
  5. Spanish Pediatric HIV Network (CoRISpe) integrated in the Spanish National AIDS Network [RIS-EPICLIN-15/2015]
  6. Instituto de Salud Carlos III
  7. Spanish Health Ministry (ISCIII-FEDER) [RD16/0025/0019]
  8. Programa de Intensificacion de Investigadores-ISCIII [INT20/00031]
  9. IISPV [2019/IISPV/05]
  10. GeSIDA
  11. Miguel Servet Program [CP19/00146]
  12. Instituto de Salud Carlos III (ISCIII) [CD20/00025]
  13. Comunidad de Madrid, Programa de Empleo Joven [PEJ-2017 AI_BMD-7446]

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This study characterized the proteomic, lipidomic, and metabolomic profiles of HIV-1-infected children based on the age at which they initiated cART. Differences in protein signatures were observed between early and late cART initiators, suggesting potential implications for metabolic disorders and non-AIDS conditions in this population. The findings underscore the importance of early antiretroviral treatment initiation in preventing long-term complications in perinatally acquired HIV-1-infected children.
Background: Early combined antiretroviral treatment (cART) in perinatally acquired HIV-1 children has been associated with a rapid viral suppression, small HIV-1 reservoir size and reduced mortality and morbidity. Immunometabolism has emerged as an important field in HIV-1 infection offering both relevant knowledge regarding immunopathogenesis and potential targets for therapies against HIV-1. Objectives: To characterize the proteomic, lipidomic and metabolomic profile of HIV-1-infected children depending on their age at cART initiation. Patients and methods: Plasma samples from perinatally HIV-1-infected children under suppressive cART who initiated an early cART (first 12 weeks after birth, EARLY, n=10) and late cART (12-50 weeks after birth, LATE, n=10) were analysed. Comparative plasma proteomics, lipidomics and metabolomics analyses were performed by nanoLC-Orbitrap, UHPLC-qTOF and GC-qTOF, respectively. Results: Seven of the 188 proteins identified exhibited differences comparing EARLY and LATE groups of HIV-1-infected children. Despite no differences in the lipidomic (n=115) and metabolomic (n=81) profiles, strong correlations were found between proteins and lipid levels as well as metabolites, including glucidic components and amino acids, with clinical parameters. The ratio among different proteins showed high discriminatory power of EARLY and LATE groups. Conclusions: Protein signature show a different proinflammatory state associated with a late cART introduction. Its associations with lipid levels and the relationships found between metabolites and clinical parameters may potentially trigger premature non-AIDS events in this HIV-1 population, including atherosclerotic diseases and metabolic disorders. Antiretroviral treatment should be started as soon as possible in perinatally acquired HIV-1-infected children to prevent them from future long-life complications.

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