eLife (Feb 2023)

Network-based multi-omics integration reveals metabolic at-risk profile within treated HIV-infection

  • Flora Mikaeloff,
  • Marco Gelpi,
  • Rui Benfeitas,
  • Andreas D Knudsen,
  • Beate Vestad,
  • Julie Høgh,
  • Johannes R Hov,
  • Thomas Benfield,
  • Daniel Murray,
  • Christian G Giske,
  • Adil Mardinoglu,
  • Marius Trøseid,
  • Susanne D Nielsen,
  • Ujjwal Neogi

DOI
https://doi.org/10.7554/eLife.82785
Journal volume & issue
Vol. 12

Abstract

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Multiomics technologies improve the biological understanding of health status in people living with HIV on antiretroviral therapy (PWH). Still, a systematic and in-depth characterization of metabolic risk profile during successful long-term treatment is lacking. Here, we used multi-omics (plasma lipidomic, metabolomic, and fecal 16 S microbiome) data-driven stratification and characterization to identify the metabolic at-risk profile within PWH. Through network analysis and similarity network fusion (SNF), we identified three groups of PWH (SNF-1–3): healthy (HC)-like (SNF-1), mild at-risk (SNF-3), and severe at-risk (SNF-2). The PWH in the SNF-2 (45%) had a severe at-risk metabolic profile with increased visceral adipose tissue, BMI, higher incidence of metabolic syndrome (MetS), and increased di- and triglycerides despite having higher CD4+ T-cell counts than the other two clusters. However, the HC-like and the severe at-risk group had a similar metabolic profile differing from HIV-negative controls (HNC), with dysregulation of amino acid metabolism. At the microbiome profile, the HC-like group had a lower α-diversity, a lower proportion of men having sex with men (MSM) and was enriched in Bacteroides. In contrast, in at-risk groups, there was an increase in Prevotella, with a high proportion of MSM, which could potentially lead to higher systemic inflammation and increased cardiometabolic risk profile. The multi-omics integrative analysis also revealed a complex microbial interplay of the microbiome-associated metabolites in PWH. Those severely at-risk clusters may benefit from personalized medicine and lifestyle intervention to improve their dysregulated metabolic traits, aiming to achieve healthier aging.

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