4.7 Article

Central nervous system (CNS) transcriptomic correlates of human immunodeficiency virus (HIV) brain RNA load in HIV-infected individuals

SCIENTIFIC REPORTS (2021)

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Journal

SCIENTIFIC REPORTS
Volume 11, Issue 1, Pages -

Publisher

NATURE RESEARCH
DOI: 10.1038/s41598-021-88052-7

Keywords

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Categories

Multidisciplinary Sciences

Funding

  1. National Institutes of Health [DA041750, DA043268, DA046170, DA046204, DA048882]
  2. NIH from the NIMH
  3. NINDS (Texas NeuroAIDS Research Center) [U24MH100930]
  4. NINDS (California NeuroAIDS Tissue Network) [U24MH100928]
  5. NINDS (National Neurological AIDS Bank) [U24MH100929]
  6. NINDS (Manhattan HIV Brain Bank) [U24MH100931]
  7. NINDS (NNTC Data Coordinating Center) [U24MH100925]

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The study revealed that brain HIV RNA load is associated with inflammation, neuronal injury, and mitochondrial dysfunction, all of which impact neuropsychological function. Potential therapeutic targets may include regulating inflammation, improving neuronal function, and restoring mitochondrial function.
To generate new mechanistic hypotheses on the pathogenesis and disease progression of neuroHIV and identify novel therapeutic targets to improve neuropsychological function in people with HIV, we investigated host genes and pathway dysregulations associated with brain HIV RNA load in gene expression profiles of the frontal cortex, basal ganglia, and white matter of HIV+ patients. Pathway analyses showed that host genes correlated with HIV expression in all three brain regions were predominantly related to inflammation, neurodegeneration, and bioenergetics. HIV RNA load directly correlated particularly with inflammation genesets representative of cytokine signaling, and this was more prominent in white matter and the basal ganglia. Increases in interferon signaling were correlated with high brain HIV RNA load in the basal ganglia and the white matter although not in the frontal cortex. Brain HIV RNA load was inversely correlated with genesets that are indicative of neuronal and synaptic genes, particularly in the cortex, indicative of synaptic injury and neurodegeneration. Brain HIV RNA load was inversely correlated with genesets that are representative of oxidative phosphorylation, electron transfer, and the tricarboxylic acid cycle in all three brain regions. Mitochondrial dysfunction has been implicated in the toxicity of some antiretrovirals, and these results indicate that mitochondrial dysfunction is also associated with productive HIV infection. Genes and pathways correlated with brain HIV RNA load suggest potential therapeutic targets to ameliorate neuropsychological functioning in people living with HIV.

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