Abstract
Accelerated neurological disorders are increasingly prominent among the HIV-infected population and are likely driven by the toxicity from long-term use of antiretroviral drugs. We explored potential side effects of antiretroviral drugs in HIV-infected primary human astrocytes and whether opioid co-exposure exacerbates the response. HIV-infected human astrocytes were exposed to the reverse transcriptase inhibitor, emtricitabine, alone or in combination with two protease inhibitors ritonavir and atazanavir (ERA) with and without morphine co-exposure. The effect of the protease inhibitor, lopinavir, alone or in combination with the protease inhibitor, abacavir, and the integrase inhibitor, raltegravir (LAR), with and without morphine co-exposure was also explored. Exposure with emtricitabine alone or ERA in HIV-infected astrocytes caused a significant decrease in viral replication and attenuated HIV-induced inflammatory molecules, while co-exposure with morphine negated the inhibitory effects of ERA, leading to increased viral replication and inflammatory molecules. Exposure with emtricitabine alone or in combination with morphine caused a significant disruption of mitochondrial membrane integrity. Genetic analysis revealed a significant increase in the expression of p62/SQSTM1 which correlated with an increase in the histone-modifying enzyme, ESCO2, after exposure with ERA alone or in combination with morphine. Furthermore, several histone-modifying enzymes such as CIITA, PRMT8, and HDAC10 were also increased with LAR exposure alone or in combination with morphine. Accumulation of p62/SQSTM1 is indicative of dysfunctional lysosomal fusion. Together with the loss of mitochondrial integrity and epigenetic changes, these effects may lead to enhanced viral titer and inflammatory molecules contributing to the neuropathology associated with HIV.
Keywords:
Antiretroviral drugs; Arginine methyl transferase; Autophagy; Opioid; Scaffold protein.
Publication types
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Research Support, N.I.H., Extramural
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Research Support, Non-U.S. Gov't
MeSH terms
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Acetyltransferases / genetics
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Acetyltransferases / metabolism
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Anti-HIV Agents / pharmacology*
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Astrocytes / drug effects*
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Astrocytes / metabolism
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Astrocytes / virology
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Atazanavir Sulfate / pharmacology
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Chromosomal Proteins, Non-Histone / genetics
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Chromosomal Proteins, Non-Histone / metabolism
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Dideoxynucleosides / pharmacology
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Drug Combinations
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Emtricitabine / pharmacology
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Gene Expression Regulation / drug effects*
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HIV-1 / drug effects
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HIV-1 / growth & development
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HIV-1 / pathogenicity
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Histone Deacetylases / genetics
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Histone Deacetylases / metabolism
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Host-Pathogen Interactions / drug effects
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Host-Pathogen Interactions / genetics
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Humans
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Lopinavir / pharmacology
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Lysosomes / drug effects
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Lysosomes / metabolism
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Lysosomes / virology
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Membrane Proteins / genetics
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Membrane Proteins / metabolism
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Mitochondria / drug effects
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Mitochondria / metabolism
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Mitochondria / virology
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Morphine / adverse effects*
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Narcotics / adverse effects*
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Nuclear Proteins / genetics
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Nuclear Proteins / metabolism
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Primary Cell Culture
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Protein-Arginine N-Methyltransferases / genetics
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Protein-Arginine N-Methyltransferases / metabolism
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Raltegravir Potassium / pharmacology
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Ritonavir / pharmacology
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Sequestosome-1 Protein / agonists
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Sequestosome-1 Protein / genetics*
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Sequestosome-1 Protein / metabolism
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Signal Transduction
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Trans-Activators / genetics
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Trans-Activators / metabolism
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Virus Replication / drug effects
Substances
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Anti-HIV Agents
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Chromosomal Proteins, Non-Histone
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Dideoxynucleosides
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Drug Combinations
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MHC class II transactivator protein
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Membrane Proteins
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Narcotics
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Nuclear Proteins
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SQSTM1 protein, human
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Sequestosome-1 Protein
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Trans-Activators
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Lopinavir
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Raltegravir Potassium
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Atazanavir Sulfate
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Morphine
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PRMT8 protein, human
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Protein-Arginine N-Methyltransferases
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Acetyltransferases
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ESCO2 protein, human
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HDAC10 protein, human
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Histone Deacetylases
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Emtricitabine
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Ritonavir
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abacavir