HIV and AIDS Malignancy Branch, National Cancer Institutegrid.48336.3a, National Institutes of Health, Bethesda, Maryland, USA.
mBio. 2021 Dec 21;12(6):e0290721. doi: 10.1128/mBio.02907-21. Epub 2021 Nov 16.
Oncogenic gammaherpesviruses express viral products during latent and lytic infection that block the innate immune response. Previously, we found that Kaposi's sarcoma herpesvirus (KSHV/human herpesvirus-8) viral microRNAs (miRNAs) downregulate cholesterol biogenesis, and we hypothesized that this prevents the production of 25-hydroxycholesterol (25HC), a cholesterol derivative. 25HC blocks KSHV infection of primary endothelial cells at a postentry step and decreases viral gene expression of LANA (latency-associated nuclear antigen) and RTA. Herein we expanded on this observation by determining transcriptomic changes associated with 25HC treatment of primary endothelial cells using RNA sequencing (RNA-Seq). We found that 25HC treatment inhibited KSHV gene expression and induced interferon-stimulated genes (ISGs) and several inflammatory cytokines (interleukin 8 [IL-8], IL-1α). Some 25HC-induced genes were partially responsible for the broadly antiviral effect of 25HC against several viruses. Additionally, we found that 25HC inhibited infection of primary B cells by a related oncogenic virus, Epstein-Barr virus (EBV/human herpesvirus-4) by suppressing key viral genes such as LMP-1 and inducing apoptosis. RNA-Seq analysis revealed that IL-1 and IL-8 pathways were induced by 25HC in both primary endothelial cells and B cells. We also found that the gene encoding cholesterol 25-hydroxylase (CH25H), which converts cholesterol to 25HC, can be induced by type I interferon (IFN) in human B cell-enriched peripheral blood mononuclear cells (PBMCs). We propose a model wherein viral miRNAs target the cholesterol pathway to prevent 25HC production and subsequent induction of antiviral ISGs. Together, these results answer some important questions about a widely acting antiviral (25HC), with implications for multiple viral and bacterial infections. A cholesterol derivative, 25-hydroxycholesterol (25HC), has been demonstrated to inhibit infections from widely different bacteria and viruses, including severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). However, its mechanism of activity is still not fully understood. In this work, we look at gene expression changes in the host and virus after 25HC treatment to find clues about its antiviral activity. We likewise demonstrate that 25HC is also antiviral against EBV, a common cancer-causing virus. We compared our results with previous data from antiviral screening assays and found the same pathways resulting in antiviral activity. Together, these results bring us closer to understanding how a modified form of cholesterol works against several viruses.
致癌性γ疱疹病毒在潜伏和裂解感染期间表达病毒产物,从而阻断先天免疫反应。此前,我们发现卡波济肉瘤疱疹病毒(KSHV/人类疱疹病毒 8)病毒 microRNAs(miRNAs)下调胆固醇生物合成,我们假设这可防止胆固醇衍生物 25-羟胆固醇(25HC)的产生。25HC 在进入后步骤中阻止 KSHV 感染原代内皮细胞,并降低 LANA(潜伏相关核抗原)和 RTA 的病毒基因表达。在此,我们通过使用 RNA 测序(RNA-Seq)确定与 25HC 处理原代内皮细胞相关的转录组变化来扩展该观察结果。我们发现,25HC 处理抑制 KSHV 基因表达,并诱导干扰素刺激基因(ISGs)和几种炎症细胞因子(白细胞介素 8 [IL-8]、IL-1α)。一些 25HC 诱导的基因部分负责 25HC 对几种病毒的广泛抗病毒作用。此外,我们发现 25HC 通过抑制关键病毒基因(如 LMP-1)的表达并诱导细胞凋亡,抑制相关致癌病毒 EBV(人类疱疹病毒 4)对原代 B 细胞的感染。RNA-Seq 分析表明,25HC 在原代内皮细胞和 B 细胞中均可诱导 IL-1 和 IL-8 通路。我们还发现,编码胆固醇 25-羟化酶(CH25H)的基因,该基因可将胆固醇转化为 25HC,可被人类富含 B 细胞的外周血单核细胞(PBMCs)中的 I 型干扰素(IFN)诱导。我们提出了一个模型,即病毒 miRNA 靶向胆固醇途径以防止 25HC 的产生和随后诱导抗病毒 ISGs。总之,这些结果回答了关于广泛作用的抗病毒物质(25HC)的一些重要问题,这对多种病毒和细菌感染具有重要意义。胆固醇衍生物 25-羟胆固醇(25HC)已被证明可抑制来自广泛不同的细菌和病毒的感染,包括严重急性呼吸综合征冠状病毒 2(SARS-CoV-2)。然而,其作用机制仍不完全清楚。在这项工作中,我们观察 25HC 处理后宿主和病毒的基因表达变化,以寻找其抗病毒活性的线索。我们同样证明 25HC 对 EBV(一种常见的致癌病毒)也具有抗病毒作用。我们将我们的结果与之前的抗病毒筛选测定结果进行了比较,发现相同的途径导致抗病毒活性。总之,这些结果使我们更接近了解一种修饰形式的胆固醇如何抵抗多种病毒。
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