病毒感染复数影响I型干扰素亚型诱导谱及干扰素刺激基因。
Virus Multiplicity of Infection Affects Type I Interferon Subtype Induction Profiles and Interferon-Stimulated Genes.
作者信息
Zaritsky Luna A, Bedsaul Jacquelyn R, Zoon Kathryn C
机构信息
Cytokine Biology Section, Division of Intramural Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland, USA.
Cytokine Biology Section, Division of Intramural Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, Maryland, USA
出版信息
J Virol. 2015 Nov;89(22):11534-48. doi: 10.1128/JVI.01727-15. Epub 2015 Sep 9.
UNLABELLED
Type I interferons (IFNs) are induced upon viral infection and important mediators of innate immunity. While there is 1 beta interferon (IFN-β) protein, there are 12 different IFN-α subtypes. It has been reported extensively that different viruses induce distinct patterns of IFN subtypes, but it has not been previously shown how the viral multiplicity of infection (MOI) can affect IFN induction. In this study, we discovered the novel finding that human U937 cells infected with 2 different concentrations of Sendai virus (SeV) induce 2 distinct type I IFN subtype profiles. Cells infected at the lower MOI induced more subtypes than cells infected at the higher MOI. We found that this was due to the extent of signaling through the IFN receptor (IFNAR). The cells infected at the lower viral MOI induced the IFNAR2-dependent IFN-α subtypes 4, 6, 7, 10, and 17, which were not induced in cells infected at higher virus concentrations. IFN-β and IFN-α1, -2, and -8 were induced in an IFNAR-independent manner in cells infected at both virus concentrations. IFN-α5, -14, -16, and -21 were induced in an IFNAR-dependent manner in cells infected at lower virus concentrations and in an IFNAR-independent manner in cells infected at higher virus concentrations. These differences in IFN subtype profiles in the 2 virus concentrations also resulted in distinct interferon-stimulated gene induction. These results present the novel finding that different viral MOIs differentially activate JAK/STAT signaling through the IFNAR, which greatly affects the profile of IFN subtypes that are induced.
IMPORTANCE
Type I IFNs are pleiotropic cytokines that are instrumental in combating viral diseases. Understanding how the individual subtypes are induced is important in developing strategies to block viral replication. Many studies have reported that different viruses induce distinct type I IFN subtype profiles due to differences in the way viruses are sensed in different cell types. However, we report in our study the novel finding that the amount of virus used to infect a system can also affect which type I IFN subtypes are induced due to the extent of activation of certain signaling pathways. These distinct IFN subtype profiles in cells infected at different MOIs are correlated with differences in interferon-stimulated gene induction, indicating that the same virus can induce distinct antiviral responses depending on the MOI. Because type I IFNs are used as therapeutic agents to treat viral diseases, understanding their antiviral mechanisms can enhance clinical treatments.
未标记
I型干扰素(IFN)在病毒感染时被诱导产生,是先天免疫的重要介质。虽然只有1种β干扰素(IFN-β)蛋白,但有12种不同的IFN-α亚型。已有大量报道称不同病毒诱导不同的IFN亚型模式,但此前尚未表明病毒感染复数(MOI)如何影响IFN诱导。在本研究中,我们发现了一个新的现象,即感染两种不同浓度仙台病毒(SeV)的人U937细胞诱导出两种不同的I型IFN亚型谱。低MOI感染的细胞比高MOI感染的细胞诱导出更多的亚型。我们发现这是由于通过IFN受体(IFNAR)的信号传导程度不同。低病毒MOI感染的细胞诱导出依赖IFNAR2的IFN-α亚型4、6、7、10和17,而高病毒浓度感染的细胞中未诱导出这些亚型。在两种病毒浓度感染的细胞中,IFN-β和IFN-α1、-2和-8以不依赖IFNAR的方式被诱导。IFN-α5、-14、-16和-21在低病毒浓度感染的细胞中以依赖IFNAR的方式被诱导,而在高病毒浓度感染的细胞中以不依赖IFNAR的方式被诱导。两种病毒浓度下IFN亚型谱的这些差异也导致了不同的干扰素刺激基因诱导。这些结果呈现了一个新的发现,即不同的病毒MOI通过IFNAR差异激活JAK/STAT信号传导,这极大地影响了诱导产生的IFN亚型谱。
重要性
I型IFN是多效性细胞因子,在对抗病毒性疾病中起作用。了解各个亚型如何被诱导对于制定阻断病毒复制的策略很重要。许多研究报道,由于在不同细胞类型中感知病毒方式的差异,不同病毒诱导不同的I型IFN亚型谱。然而,我们在研究中报道了一个新的发现,即用于感染系统的病毒量也会由于某些信号通路激活程度的不同而影响诱导产生的I型IFN亚型。在不同MOI感染的细胞中这些不同的IFN亚型谱与干扰素刺激基因诱导的差异相关,表明相同病毒根据MOI可诱导不同的抗病毒反应。由于I型IFN被用作治疗病毒性疾病的药物,了解它们的抗病毒机制可以加强临床治疗。
Zotero 插件