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Cannabidiol Modulates Expression of Type I IFN Response Genes and HIV Infection in Macrophages.

Frontiers in immunology(2022)SCI 2区

Univ Calif Los Angeles UCLA

Cited 7|Views28
Abstract
Cannabis (Cannabis sativa) is a widely used drug in the United States and the frequency of cannabis use is particularly high among people living with HIV (PLWH). One key component of cannabis, the non-psychotropic (−)-cannabidiol (CBD) exerts a wide variety of biological actions, including anticonvulsive, analgesic, and anti-inflammatory effects. However, the exact mechanism of action through which CBD affects the immune cell signaling remains poorly understood. Here we report that CBD modulates type I interferon responses in human macrophages. Transcriptomics analysis shows that CBD treatment significantly attenuates cGAS-STING-mediated activation of type I Interferon response genes (ISGs) in monocytic THP-1 cells. We further showed that CBD treatment effectively attenuates 2’3-cGAMP stimulation of ISGs in both THP-1 cells and primary human macrophages. Interestingly, CBD significantly upregulates expression of autophagy receptor p62/SQSTM1. p62 is critical for autophagy-mediated degradation of stimulated STING. We observed that CBD treated THP-1 cells have elevated autophagy activity. Upon 2’3’-cGAMP stimulation, CBD treated cells have rapid downregulation of phosphorylated-STING, leading to attenuated expression of ISGs. The CBD attenuation of ISGs is reduced in autophagy deficient THP-1 cells, suggesting that the effects of CBD on ISGs is partially mediated by autophagy induction. Lastly, CBD decreases ISGs expression upon HIV infection in THP-1 cells and human primary macrophages, leading to increased HIV RNA expression 24 hours after infection. However, long term culture with CBD in infected primary macrophages reduced HIV viral spread, suggesting potential dichotomous roles of CBD in HIV replication. Our study highlights the immune modulatory effects of CBD and the needs for additional studies on its effect on viral infection and inflammation.
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HIV,human immunodeficiency virus,CBD,cannabidiol,ISG (interferon stimulated genes),type I interferons,macrophage
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要点】:本研究揭示了非psychoactive的Cannabis成分CBD如何调节HIV感染的人体巨噬细胞中的type I interferon反应基因表达,指出CBD通过增强自噬过程来抑制cGAS-STING途径的激活,进而影响ISGs表达,这对HIV感染有重要影响。

方法】:本研究采用了转录组学分析,对CBD处理的人单核细胞系THP-1和原代人巨噬细胞进行了研究。

实验】:研究发现CBD能显著降低cGAMP刺激的ISGs在THP-1细胞和原发性人类巨噬细胞中的表达。CBD处理增加了自噬受体p62/SQSTM1的表达,促进了STING的降解,降低了ISGs的表达。此外,在HIV感染的情况下,CBD降低了THP-1细胞和原发性人类巨噬细胞中ISGs的表达,增加了24小时后的HIV RNA表达,但在长期培养中,CBD降低了感染的巨噬细胞中的HIV病毒传播,表明CBD在HIV复制中具有潜在的二元作用。