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HIV-1 and opiates modulate miRNA profiles in extracellular vesicles. | LitMetric

AI Article Synopsis

  • Opiate abuse is linked to a higher risk of HIV transmission and worsens HIV-related nerve damage by affecting inflammation and immune responses.
  • This study focuses on the development of a unique exosomal miRNA biomarker profile for HIV-infected cells, specifically looking at how morphine influences these miRNAs.
  • Findings indicate that HIV and morphine together alter miRNA levels, which can impact neuronal function, suggesting potential new targets for treatment or understanding the disease mechanisms.

Article Abstract

Opiate abuse increases the risk of HIV transmission and exacerbates HIV neuropathology by increasing inflammation and modulating immune cell function. Exosomal EVs(xEV) contain miRNAs that may be differentially expressed due to HIV infection or opiate abuse. Here we develop a preliminary exosomal-miRNA biomarker profile of HIV-infected PBMCs in the context of opiate use. PBMCs infected with HIV were treated with increasing dosages of morphine for 72 hours, the culture supernatants were collected, and the exosomes isolated using differential centrifugation. Exosomal miRNAs were extracted, expression levels determined via Nanostring multiplexed microRNA arrays, and analyzed with Webgestalt. The effect of the exosomes on neuronal function was determined by measuring calcium. Preliminary findings show that HIV-1 infection altered the miRNA profile of PBMC-derived EVs concurrently with opiate exposure. MicroRNA, hsa-miR-1246 was up-regulated 12-fold in the presence of morphine, relative to uninfected control. PBMCs infected with HIV-1 MN, an X4-tropic HIV-1 strain and exposed to morphine, displayed a trend which suggests potential synergistic effects between HIV-1 infection and morphine exposure promoting an increase in viral replication. Dose-dependent differences were observed in miRNA expression as a result of opiate exposure. The xEVs derived from PBMCs exposed to morphine or HIV modulated neuronal cell function. SH-SY5Y cells, treated with xEVs derived from ART-treated PBMCs, exhibited increased viability while for SH-SY5Ys exposed to xEVs derived from HIV-1 infected PBMCs viability was decreased compared to the untreated control. Exposing SH-SY5Y to xEVs derived from HIV-infected PBMCs resulted in significant decrease in calcium signaling, relative to treatment with xEVs derived from uninfected PBMCs. Overall, HIV-1 and morphine induced differential miRNA expression in PBMC-derived exosomes, potentially identifying mechanisms of action or novel therapeutic targets involved in opiate use disorder, HIV neuropathology, TNF signaling pathway, NF-κB signaling pathway, autophagy, and apoptosis in context of HIV infection.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10666642PMC
http://dx.doi.org/10.3389/fimmu.2023.1259998DOI Listing

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Article Synopsis
  • Opiate abuse is linked to a higher risk of HIV transmission and worsens HIV-related nerve damage by affecting inflammation and immune responses.
  • This study focuses on the development of a unique exosomal miRNA biomarker profile for HIV-infected cells, specifically looking at how morphine influences these miRNAs.
  • Findings indicate that HIV and morphine together alter miRNA levels, which can impact neuronal function, suggesting potential new targets for treatment or understanding the disease mechanisms.
View Article and Find Full Text PDF

Exosomal extracellular vesicles (xEVs) in plasma and cerebrospinal fluid (CSF) of aviremic people living with HIV/AIDS (PLWHA) contain the HIV Negative factor (Nef) protein. However, the role of xEVs and Nef-containing-xEVs(xEV-Nef) in HIV-associated neuropathology is unknown. Here we performed a cross-sectional analysis of the content of xEVs derived from matched serum and CSF samples of PLWHAs diagnosed with either asymptomatic neurocognitive impairment (ANI), mild neurocognitive disorder (MND), or HIV-associated dementia (HAD).

View Article and Find Full Text PDF

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