Inhibition of Zika Virus by hybrid interferons
混合干扰素对寨卡病毒的抑制作用
基本信息
- 批准号:2907794
- 负责人:
- 金额:--
- 依托单位:
- 依托单位国家:英国
- 项目类别:Studentship
- 财政年份:2023
- 资助国家:英国
- 起止时间:2023 至 无数据
- 项目状态:未结题
- 来源:
- 关键词:
项目摘要
Zika Virus (ZIKV) is a re-emerging mosquito-borne flavivirus. In most cases ZIKV infection is mild and resolve on their own. However, ZIKV is also linked to developmental abnormalities in foetuses including microcephaly and other serious neurological diseases like Guillain-Barre syndrome in adults. Despite being declared an international health emergency, we have no specific treatment or vaccine available for ZIKV infection.Interferons (IFNs) are our bodies first line defence against viruses. Depending on their receptor usage IFNs are divided into three types, type 1, 2 and 3 IFNs. They control viral infection by inducing the expression of antiviral proteins that are encoded by interferon-stimulated genes (ISGs). The initial host response against virus infection is the induction of type 1 IFNs. There are 12 human IFN alpha (a type 1 IFN) subtypes but only IFNa 2a and 2b subtypes are used clinically. They have been approved by the FDA for the treatment of certain infections and cancers including chronic Hepatitis C, AIDS-related Kaposi sarcoma, hairy cell leukaemia, and hepatitis B in adults. However, studies have shown that IFNa 2 subtypes have weaker antiviral activity as compared to other more potent IFNa subtypes. For instance, IFNa 14 has been shown to be highly active against viruses including HIV and influenza A virus. Working with our industrial partner ILC Therapeutics, we have access to novel hybrid interferons alongside in-house synthetic and naturally occurring IFNa variants that are based on the IFNa 14 backbone. This study aims to test if the IFNa 14 and its derivatives have antiviral activity against ZIKV infection. To do this, we aim to test different IFNa subtypes and their synthetic derivatives for their inhibition of different lineage ZIKV utilising plaque assays, reporter assays and qPCRs. We will also aim to identify the different interferon stimulated genes (ISGs) that are differentially expressed in cells stimulated with different IFNa subtypes using RNA-Seq analysis and to validate the identified ISGs with qPCR and pulse SILAC proteomic analyses. This study will also generate ISG overexpression cell lines and knock-out cells lines to test for their sensitivity and resistance to ZIKV; and to determine the role of the ZIKV protein NS5 in counteracting the antiviral activity of the different IFNa subtypes. This will enable us to understand how hybrid interferons might control ZIKV infection and reveal the differences in therapeutic responsiveness according to viral genotype.
寨卡病毒(ZIKV)是一种由蚊子传播的黄病毒。在大多数情况下,ZIKV感染是轻微的,并自行解决。然而,ZIKV也与胎儿的发育异常有关,包括小头畸形和其他严重的神经系统疾病,如成年人的格林-巴利综合征。尽管已被宣布为国际卫生紧急情况,但我们没有针对ZIKV感染的特异性治疗或疫苗。干扰素(IFN)是我们身体对抗病毒的第一道防线。根据其受体用途,IFN分为三种类型,1型、2型和3型IFN。它们通过诱导由干扰素刺激基因(ISG)编码的抗病毒蛋白的表达来控制病毒感染。针对病毒感染的初始宿主应答是诱导1型IFN。人IFN α(1型IFN)有12种亚型,但临床上仅使用IFNa 2a和2b亚型。它们已被FDA批准用于治疗某些感染和癌症,包括慢性丙型肝炎、艾滋病相关的卡波西肉瘤、毛细胞白血病和成人B型肝炎。然而,研究表明,与其他更有效的IFNa亚型相比,IFNa 2亚型具有较弱的抗病毒活性。例如,IFNa 14已被证明对包括HIV和甲型流感病毒在内的病毒具有高度活性。与我们的工业合作伙伴ILC Therapeutics合作,我们可以获得新型混合干扰素以及基于IFNa 14骨架的内部合成和天然存在的IFNa变体。本研究旨在测试IFNa 14及其衍生物是否具有针对ZIKV感染的抗病毒活性。为此,我们旨在利用噬斑测定、报告基因测定和qPCR测试不同的IFNa亚型及其合成衍生物对不同谱系ZIKV的抑制。我们还将旨在使用RNA-Seq分析鉴定在用不同IFNa亚型刺激的细胞中差异表达的不同干扰素刺激的基因(ISG),并使用qPCR和脉冲SILAC蛋白质组学分析验证鉴定的ISG。本研究还将产生ISG过表达细胞系和敲除细胞系,以测试它们对ZIKV的敏感性和抗性;并确定ZIKV蛋白NS 5在抵消不同IFNa亚型的抗病毒活性中的作用。这将使我们能够了解杂交干扰素如何控制ZIKV感染,并揭示根据病毒基因型的治疗反应性差异。
项目成果
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其他文献
吉治仁志 他: "トランスジェニックマウスによるTIMP-1の線維化促進機序"最新医学. 55. 1781-1787 (2000)
Hitoshi Yoshiji 等:“转基因小鼠中 TIMP-1 的促纤维化机制”现代医学 55. 1781-1787 (2000)。
- DOI:
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LiDAR Implementations for Autonomous Vehicle Applications
- DOI:
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2021 - 期刊:
- 影响因子:0
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吉治仁志 他: "イラスト医学&サイエンスシリーズ血管の分子医学"羊土社(渋谷正史編). 125 (2000)
Hitoshi Yoshiji 等人:“血管医学与科学系列分子医学图解”Yodosha(涉谷正志编辑)125(2000)。
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Effect of manidipine hydrochloride,a calcium antagonist,on isoproterenol-induced left ventricular hypertrophy: "Yoshiyama,M.,Takeuchi,K.,Kim,S.,Hanatani,A.,Omura,T.,Toda,I.,Akioka,K.,Teragaki,M.,Iwao,H.and Yoshikawa,J." Jpn Circ J. 62(1). 47-52 (1998)
钙拮抗剂盐酸马尼地平对异丙肾上腺素引起的左心室肥厚的影响:“Yoshiyama,M.,Takeuchi,K.,Kim,S.,Hanatani,A.,Omura,T.,Toda,I.,Akioka,
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