小鼠鸟苷结合蛋白1在体内或体外均不介导对流感病毒的抗病毒活性

IF 3.2 4区 医学 Q3 CELL BIOLOGY Immunology & Cell Biology Pub Date : 2023-02-06 DOI:10.1111/imcb.12627
Melkamu B Tessema, Daniel Enosi Tuipulotu, Clare V Oates, Andrew G Brooks, Si Ming Man, Sarah L Londrigan, Patrick C Reading
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引用次数: 1

摘要

许多干扰素(IFN)刺激的基因在感染流感和其他病毒后在宿主细胞内上调。虽然一些ifn刺激基因的抗病毒活性,如ifn诱导的GTPase黏液瘤抗性(Mx)1蛋白1,已经被很好地定义,但关于鸟苷酸结合蛋白(GBP)家族中相关ifn诱导的GTPase的抗病毒活性,特别是小鼠GBPs,人们对其抗病毒活性知之甚少,小鼠模型可用于评估其体内抗病毒特性。本研究表明,在小鼠气道上皮细胞系(LA-4细胞)中,经小鼠IFNα预处理或感染甲型流感病毒(IAV)后,小鼠GBP1 (mGBP1)表达上调。多西环素诱导的小鼠Mx1 (mMx1)在LA-4细胞中的表达降低了对IAV感染的易感性并降低了病毒生长,而诱导的mGBP1则没有。此外,从mGBP1缺陷小鼠(mGBP1−/−)分离的原代细胞对IAV的易感性没有差异,mGBP1−/−巨噬细胞在IAV诱导的NLRP3 (NLR家族pyrin结构域含3)炎症小体激活中没有缺陷。在鼻内IAV感染后,mGBP1 - / -小鼠在感染期间气道内的病毒复制或炎症反应诱导方面也没有表现出差异。因此,通过mGBP1过表达、mGBP1 - / -小鼠细胞和mGBP1 - / -鼻内感染等互补方法,我们证明了mGBP1在体外或体内调节IAV感染中并不起主要作用。
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Mouse guanylate-binding protein 1 does not mediate antiviral activity against influenza virus in vitro or in vivo

Many interferon (IFN)-stimulated genes are upregulated within host cells following infection with influenza and other viruses. While the antiviral activity of some IFN-stimulated genes, such as the IFN-inducible GTPase myxoma resistance (Mx)1 protein 1, has been well defined, less is known regarding the antiviral activities of related IFN-inducible GTPases of the guanylate-binding protein (GBP) family, particularly mouse GBPs, where mouse models can be used to assess their antiviral properties in vivo. Herein, we demonstrate that mouse GBP1 (mGBP1) was upregulated in a mouse airway epithelial cell line (LA-4 cells) following pretreatment with mouse IFNα or infection by influenza A virus (IAV). Whereas doxycycline-inducible expression of mouse Mx1 (mMx1) in LA-4 cells resulted in reduced susceptibility to IAV infection and reduced viral growth, inducible mGBP1 did not. Moreover, primary cells isolated from mGBP1-deficient mice (mGBP1−/−) showed no difference in susceptibility to IAV and mGBP1−/− macrophages showed no defect in IAV-induced NLRP3 (NLR family pyrin domain containing 3) inflammasome activation. After intranasal IAV infection, mGBP1−/− mice also showed no differences in virus replication or induction of inflammatory responses in the airways during infection. Thus, using complementary approaches such as mGBP1 overexpression, cells from mGBP1−/− mice and intranasal infection of mGBP1−/− we demonstrate that mGBP1 does not play a major role in modulating IAV infection in vitro or in vivo.

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来源期刊
Immunology & Cell Biology
Immunology & Cell Biology 医学-免疫学
CiteScore
7.50
自引率
2.50%
发文量
98
审稿时长
4-8 weeks
期刊介绍: The Australasian Society for Immunology Incorporated (ASI) was created by the amalgamation in 1991 of the Australian Society for Immunology, formed in 1970, and the New Zealand Society for Immunology, formed in 1975. The aim of the Society is to encourage and support the discipline of immunology in the Australasian region. It is a broadly based Society, embracing clinical and experimental, cellular and molecular immunology in humans and animals. The Society provides a network for the exchange of information and for collaboration within Australia, New Zealand and overseas. ASI members have been prominent in advancing biological and medical research worldwide. We seek to encourage the study of immunology in Australia and New Zealand and are active in introducing young scientists to the discipline.
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