Sequence Diversity in the 3' Untranslated Region of Alphavirus Modulates IFIT2-Dependent Restriction in a Cell Type-Dependent Manner.

IF 1.9 4区医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY

Journal of Interferon and Cytokine Research Pub Date : 2025-04-01 Epub Date: 2025-03-12 DOI:10.1089/jir.2024.0229

Sarah E Hickson, Eden Brekke, Johannes Schwerk, Indraneel Saluhke, Shivam Zaver, Joshua Woodward, Ram Savan, Jennifer L Hyde

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引用次数: 0

Abstract

Alphaviruses (family Togaviridae) are a diverse group of positive-sense RNA (+ssRNA) viruses that are transmitted by arthropods and are the causative agent of several significant human and veterinary diseases. Interferon (IFN)-induced proteins with tetratricopeptide repeats (IFITs) are a family of RNA-binding IFN-stimulated genes (ISGs) that are highly upregulated following viral infection and have been identified as potential restrictors of alphaviruses. The mechanism by which IFIT1 restricts RNA viruses is dependent on self and non-self-discrimination of RNA, and alphaviruses evade this recognition via their 5' untranslated region (UTR). However, the role of IFIT2 during alphavirus replication and the mechanism of viral replication inhibition is unclear. In this study, we identify IFIT2 as a restriction factor for Venezuelan equine encephalitis virus (VEEV) and show that IFIT2 binds the 3' 3'UTR of the virus. We investigated the potential role of variability in the 3'UTR of the virus affecting IFIT2 antiviral activity by studying infection with VEEV. Comparison of recombinant VEEV clones containing 3'UTR sequences derived from epizootic and enzootic isolates exhibited differential sensitivity to IFIT2 restriction in vitro infection studies, suggesting that the alphavirus 3'UTR sequence may function in part to evade IFIT2 restriction. In vitro binding assays demonstrate that IFIT2 binds to the VEEV 3'UTR; however, in contrast to previous studies, VEEV restriction did not appear to be dependent on the ability of IFIT2 to inhibit translation of viral RNA, suggesting a novel mechanism of IFIT2 restriction. Our study demonstrates that IFIT2 is a restriction factor for alphaviruses and variability in the 3'UTR of VEEV can modulate viral restriction by IFIT2. Ongoing studies are exploring the biological consequences of IFIT2-VEEV RNA interaction in viral pathogenesis and defining sequence and structural features of RNAs that regulate IFIT2 recognition.

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甲病毒3'非翻译区的序列多样性以细胞类型依赖的方式调节ifit2依赖性限制。

甲病毒（毒虫病毒科）是一种多样的正义RNA （+ssRNA）病毒，通过节肢动物传播，是几种重要的人类和兽医疾病的病原体。干扰素（IFN）诱导蛋白与四肽重复序列（IFITs）是一个rna结合干扰素刺激基因（ISGs）家族，在病毒感染后高度上调，并已被确定为甲病毒的潜在限制性因子。IFIT1限制RNA病毒的机制依赖于RNA的自我和非自我识别，而甲病毒通过其5'非翻译区（UTR）逃避这种识别。然而，IFIT2在甲病毒复制过程中的作用和抑制病毒复制的机制尚不清楚。在这项研究中，我们确定IFIT2是委内瑞拉马脑炎病毒（VEEV）的一个限制性因子，并表明IFIT2与该病毒的3' 3' utr结合。通过研究VEEV感染，我们研究了病毒3'UTR变异性影响IFIT2抗病毒活性的潜在作用。在体外感染研究中，来自兽疫分离株和兽疫分离株的含有3'UTR序列的重组VEEV克隆对IFIT2限制的敏感性存在差异，这表明甲型病毒的3'UTR序列可能在一定程度上逃避了IFIT2限制。体外结合实验表明，IFIT2与veev3 ' utr结合；然而，与先前的研究相反，VEEV限制似乎并不依赖于IFIT2抑制病毒RNA翻译的能力，这表明IFIT2限制的新机制。我们的研究表明，IFIT2是甲病毒的限制性因子，VEEV 3'UTR的变异性可以调节IFIT2对病毒的限制性。正在进行的研究正在探索IFIT2- veev RNA相互作用在病毒发病机制中的生物学后果，并确定调节IFIT2识别的RNA的序列和结构特征。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Interferon and Cytokine Research 医学-免疫学

CiteScore

3.80

自引率

0.00%

发文量

审稿时长

2.2 months

期刊介绍： Journal of Interferon & Cytokine Research (JICR) provides the latest groundbreaking research on all aspects of IFNs and cytokines. The Journal delivers current findings on emerging topics in this niche community, including the role of IFNs in the therapy of diseases such as multiple sclerosis, the understanding of the third class of IFNs, and the identification and function of IFN-inducible genes.