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The ubiquitin E3 ligase RAUL negatively regulates type i interferon through ubiquitination of the transcription factors IRF7 and IRF3.泛素 E3 连接酶 RAUL 通过泛素化转录因子 IRF7 和 IRF3 负调控 I 型干扰素。
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Self protection from anti-viral responses--Ro52 promotes degradation of the transcription factor IRF7 downstream of the viral Toll-Like receptors.自身对抗病毒反应的保护——Ro52 促进了病毒 Toll 样受体下游转录因子 IRF7 的降解。
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The transcription factor MafB antagonizes antiviral responses by blocking recruitment of coactivators to the transcription factor IRF3.转录因子 MafB 通过阻止共激活因子募集到转录因子 IRF3 上来拮抗抗病毒反应。
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IRF7:激活、调控、修饰和功能。

IRF7: activation, regulation, modification and function.

机构信息

Division of Hematology/Oncology, Department of Medicine, Viral Oncology Program, Sylvester Comprehensive Cancer Center, Miller School of Medicine, University of Miami, Miami, FL 33136, USA.

出版信息

Genes Immun. 2011 Sep;12(6):399-414. doi: 10.1038/gene.2011.21. Epub 2011 Apr 14.

DOI:10.1038/gene.2011.21
PMID:21490621
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4437765/
Abstract

Interferon regulatory factor 7 (IRF7) was originally identified in the context of Epstein-Barr virus (EBV) infection, and has since emerged as the crucial regulator of type I interferons (IFNs) against pathogenic infections, which activate IRF7 by triggering signaling cascades from pathogen recognition receptors (PRRs) that recognize pathogenic nucleic acids. Moreover, IRF7 is a multifunctional transcription factor, underscored by the fact that it is associated with EBV latency, in which IRF7 is induced as well as activated by the EBV principal oncoprotein latent membrane protein-1 (LMP1). Aberrant production of type I IFNs is associated with many types of diseases such as cancers and autoimmune disorders. Thus, tight regulation of IRF7 expression and activity is imperative in dictating appropriate type I IFN production for normal IFN-mediated physiological functions. Posttranslational modifications have important roles in regulation of IRF7 activity, exemplified by phosphorylation, which is indicative of its activation. Furthermore, mounting evidence has shed light on the importance of regulatory ubiquitination in activation of IRF7. Albeit these exciting findings have been made in the past decade since its discovery, many questions related to IRF7 remain to be addressed.

摘要

干扰素调节因子 7 (IRF7) 最初是在 EBV(Epstein-Barr virus)感染的背景下被发现的,此后成为对抗致病性感染的 I 型干扰素 (IFN) 的关键调节剂,通过触发识别病原体核酸的病原体识别受体 (PRR) 的信号级联反应来激活 IRF7。此外,IRF7 是一种多功能转录因子,这一点很重要,因为它与 EBV 潜伏期有关,在 EBV 潜伏期,IRF7 被 EBV 主要癌蛋白潜伏膜蛋白-1 (LMP1) 诱导和激活。I 型 IFN 的异常产生与许多疾病有关,如癌症和自身免疫性疾病。因此,严格调控 IRF7 的表达和活性对于决定适当的 I 型 IFN 产生以实现正常的 IFN 介导的生理功能至关重要。翻译后修饰在调节 IRF7 活性方面起着重要作用,例如磷酸化,它是其激活的标志。此外,越来越多的证据表明,调节泛素化在激活 IRF7 方面的重要性。尽管自发现以来的过去十年中取得了这些令人兴奋的发现,但仍有许多与 IRF7 相关的问题需要解决。