Retrovirology (Jun 2011)

Interactions between human immunodeficiency virus (HIV)-1 Vpr expression and innate immunity influence neurovirulence

  • Ballanyi Klaus,
  • Maingat Ferdinand,
  • McFarlane Nicola,
  • Noorbakhsh Farshid,
  • Vivithanaporn Pornpun,
  • Jones Gareth,
  • Acharjee Shaona,
  • Na Hong,
  • Pardo Carlos A,
  • Cohen Éric A,
  • Power Christopher

DOI
https://doi.org/10.1186/1742-4690-8-44
Journal volume & issue
Vol. 8, no. 1
p. 44

Abstract

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Abstract Background Viral diversity and abundance are defining properties of human immunodeficiency virus (HIV)-1's biology and pathogenicity. Despite the increasing availability of antiretroviral therapy, HIV-associated dementia (HAD) continues to be a devastating consequence of HIV-1 infection of the brain although the underlying disease mechanisms remain uncertain. Herein, molecular diversity within the HIV-1 non-structural gene, Vpr, was examined in RNA sequences derived from brain and blood of HIV/AIDS patients with or without HIV-associated dementia (HAD) together with the ensuing pathobiological effects. Results Cloned brain- and blood-derived full length vpr alleles revealed that amino acid residue 77 within the brain-derived alleles distinguished HAD (77Q) from non-demented (ND) HIV/AIDS patients (77R) (p vpr transcripts were more frequently detected in HAD brains (p IFN-α, MX1 and BST-2 transcript levels in human glia relative to the 77Q-HAD encoding virus (p Vpr77Q-HAD), 77R (pVpr77R-ND) or Vpr null (pVpr(-))-containing vectors showed that the pVpr77R-ND vector induced higher levels of immune gene expression (p p IFN-α, MX1, PRKRA and BST-2 relative to 77Q-HAD peptide (p p p Conclusions These observations underscored the potent neuropathogenic properties of Vpr but also indicated viral diversity modulates innate neuroimmunity and neurodegeneration.