PLoS Pathogens (Mar 2023)

Chronic immune activation and gut barrier dysfunction is associated with neuroinflammation in ART-suppressed SIV+ rhesus macaques.

  • Sarah J Byrnes,
  • Kathleen Busman-Sahay,
  • Thomas A Angelovich,
  • Skyler Younger,
  • Sol Taylor-Brill,
  • Michael Nekorchuk,
  • Stephen Bondoc,
  • Rachel Dannay,
  • Margaret Terry,
  • Catherine R Cochrane,
  • Trisha A Jenkins,
  • Michael Roche,
  • Claire Deleage,
  • Steven E Bosinger,
  • Mirko Paiardini,
  • Bruce J Brew,
  • Jacob D Estes,
  • Melissa J Churchill

DOI
https://doi.org/10.1371/journal.ppat.1011290
Journal volume & issue
Vol. 19, no. 3
p. e1011290

Abstract

Read online

HIV-associated neurocognitive disorders (HAND) affect ~40% of virally suppressed people with HIV (PWH), however, the precise viral dependent and independent changes to the brain are unclear. Here we characterized the CNS reservoir and immune environment of SIV-infected (SIV+) rhesus macaques during acute (n = 4), chronic (n = 12) or ART-suppressed SIV infection (n = 11). Multiplex immunofluorescence for markers of SIV infection (vRNA/vDNA) and immune activation was performed on frontal cortex and matched colon tissue. SIV+ animals contained detectable viral DNA+ cells that were not reduced in the frontal cortex or the gut by ART, supporting the presence of a stable viral reservoir in these compartments. SIV+ animals had impaired blood brain barrier (BBB) integrity and heightened levels of astrocytes or myeloid cells expressing antiviral, anti-inflammatory or oxidative stress markers which were not abrogated by ART. Neuroinflammation and BBB dysfunction correlated with measures of viremia and immune activation in the gut. Furthermore, SIV-uninfected animals with experimentally induced gut damage and colitis showed a similar immune activation profile in the frontal cortex to those of SIV-infected animals, supporting the role of chronic gut damage as an independent source of neuroinflammation. Together, these findings implicate gut-associated immune activation/damage as a significant contributor to neuroinflammation in ART-suppressed HIV/SIV infection which may drive HAND pathogenesis.