感染传染性法氏囊病病毒时宿主反应中 NR2F2 表达减少通过靶向 SOCS5 增强 I 型干扰素表达抑制病毒复制。
Reduced NR2F2 Expression in the Host Response to Infectious Bursal Disease Virus Infection Suppressed Viral Replication by Enhancing Type I Interferon Expression by Targeting SOCS5.
机构信息
National Key Laboratory of Veterinary Public Health Security, College of Veterinary Medicine, China Agricultural University, Beijing, China.
Animal Epidemiology of the Ministry of Agriculture, College of Veterinary Medicine, China Agricultural University, Beijing, China.
出版信息
J Virol. 2023 Jul 27;97(7):e0066423. doi: 10.1128/jvi.00664-23. Epub 2023 Jun 26.
Nuclear receptors are ligand-activated transcription factors that play an important role in regulating innate antiviral immunity and other biological processes. However, the role of nuclear receptors in the host response to infectious bursal disease virus (IBDV) infection remains elusive. In this study, we show that IBDV infection or poly(I·C) treatment of DF-1 or HD11 cells markedly decreased nuclear receptor subfamily 2 group F member 2 (NR2F2) expression. Surprisingly, knockdown, knockout, or inhibition of NR2F2 expression in host cells remarkably inhibited IBDV replication and promoted IBDV/poly(I·C)-induced type I interferon and interferon-stimulated genes expression. Furthermore, our data show that NR2F2 negatively regulates the antiviral innate immune response by promoting the suppressor of cytokine signaling 5 (SOCS5) expression. Thus, reduced NR2F2 expression in the host response to IBDV infection inhibited viral replication by enhancing the expression of type I interferon by targeting SOCS5. These findings reveal that NR2F2 plays a crucial role in antiviral innate immunity, furthering our understanding of the mechanism underlying the host response to viral infection. Infectious bursal disease (IBD) is an immunosuppressive disease causing considerable economic losses to the poultry industry worldwide. Nuclear receptors play an important role in regulating innate antiviral immunity. However, the role of nuclear receptors in the host response to IBD virus (IBDV) infection remains elusive. Here, we report that NR2F2 expression decreased in IBDV-infected cells, which consequently reduced SOCS5 expression, promoted type I interferon expression, and suppressed IBDV infection. Thus, NR2F2 serves as a negative factor in the host response to IBDV infection by regulating SOCS5 expression, and intervention in the NR2F2-mediated host response by specific inhibitors might be employed as a strategy for prevention and treatment of IBD.
核受体是配体激活的转录因子,在调节先天抗病毒免疫和其他生物学过程中发挥重要作用。然而,核受体在宿主对传染性法氏囊病病毒(IBDV)感染的反应中的作用仍不清楚。在这项研究中,我们表明,IBDV 感染或多聚(I·C)处理 DF-1 或 HD11 细胞显著降低了核受体亚家族 2 组 F 成员 2(NR2F2)的表达。令人惊讶的是,宿主细胞中 NR2F2 的敲低、敲除或抑制显著抑制了 IBDV 的复制,并促进了 IBDV/多聚(I·C)诱导的 I 型干扰素和干扰素刺激基因的表达。此外,我们的数据表明,NR2F2 通过促进细胞因子信号转导抑制因子 5(SOCS5)的表达来负调控抗病毒先天免疫反应。因此,宿主对 IBDV 感染的反应中 NR2F2 表达的减少通过靶向 SOCS5 增强 I 型干扰素的表达来抑制病毒复制。这些发现揭示了 NR2F2 在抗病毒先天免疫中发挥关键作用,进一步了解了宿主对病毒感染的反应机制。传染性法氏囊病(IBD)是一种免疫抑制性疾病,给全球家禽业造成了巨大的经济损失。核受体在调节先天抗病毒免疫中发挥重要作用。然而,核受体在宿主对 IBD 病毒(IBDV)感染的反应中的作用仍不清楚。在这里,我们报告 NR2F2 的表达在 IBDV 感染的细胞中降低,这导致 SOCS5 的表达减少,促进了 I 型干扰素的表达,并抑制了 IBDV 的感染。因此,NR2F2 通过调节 SOCS5 的表达成为宿主对 IBDV 感染反应的负性因子,通过特异性抑制剂干预 NR2F2 介导的宿主反应可能成为预防和治疗 IBD 的策略。
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