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Opposing Roles of Double-Stranded RNA Effector Pathways and Viral Defense Proteins Revealed with CRISPR-Cas9 Knockout Cell Lines and Vaccinia Virus Mutants.利用CRISPR-Cas9基因敲除细胞系和痘苗病毒突变体揭示双链RNA效应途径和病毒防御蛋白的相反作用
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A forward genetic screen reveals novel independent regulators of ULBP1, an activating ligand for natural killer cells.一项正向遗传学筛选揭示了ULBP1(一种自然杀伤细胞激活配体)新的独立调节因子。
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Protein kinase IKKβ-catalyzed phosphorylation of IRF5 at Ser462 induces its dimerization and nuclear translocation in myeloid cells.蛋白激酶IKKβ催化的IRF5在丝氨酸462处的磷酸化诱导其在髓系细胞中的二聚化和核转位。
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Altered microRNA expression after infection with human cytomegalovirus leads to TIMP3 downregulation and increased shedding of metalloprotease substrates, including MICA.人巨细胞病毒感染后微小 RNA 表达改变导致 TIMP3 下调和金属蛋白酶底物(包括 MICA)的释放增加。
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RAE1 ligands for the NKG2D receptor are regulated by STING-dependent DNA sensor pathways in lymphoma.淋巴瘤中 NKG2D 受体的 RAE1 配体受 STING 依赖性 DNA 传感器途径的调控。
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病毒感染后,双链RNA的天然免疫识别会触发NKG2D配体表达增加。

Innate immune recognition of double-stranded RNA triggers increased expression of NKG2D ligands after virus infection.

作者信息

Esteso Gloria, Guerra Susana, Valés-Gómez Mar, Reyburn Hugh T

机构信息

From the Department of Immunology and Oncology, Centro Nacional de Biotecnología/Consejo Superior de Investigaciones Científicas (CNB-CSIC), 28049 Madrid and.

the Department of Preventive Medicine and Public Health, Universidad Autónoma, 28029 Madrid, Spain.

出版信息

J Biol Chem. 2017 Dec 15;292(50):20472-20480. doi: 10.1074/jbc.M117.818393. Epub 2017 Oct 6.

DOI:10.1074/jbc.M117.818393
PMID:28986447
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5733586/
Abstract

Self/non-self-discrimination by the innate immune system relies on germline-encoded, non-rearranging receptors expressed by innate immune cells recognizing conserved pathogen-associated molecular patterns. The natural killer group 2D (NKG2D) receptor is a potent immune-activating receptor that binds human genome-encoded ligands, whose expression is negligible in normal tissues, but increased in stress and disease conditions for reasons that are incompletely understood. Here it is not clear how the immune system reconciles receptor binding of self-proteins with self/non-self-discrimination to avoid autoreactivity. We now report that increased expression of NKG2D ligands after virus infection depends on interferon response factors activated by the detection of viral double-stranded RNA by pattern-recognition receptors (RIG-I/MDA-5) and that NKG2D ligand up-regulation can be blocked by the expression of viral dsRNA-binding proteins. Thus, innate immunity-mediated recognition of viral nucleic acids triggers the infected cell to release interferon for NK cell recruitment and to express NKG2D ligands to become more visible to the immune system. Finally, the observation that NKG2D-ligand induction is a consequence of signaling by pattern-recognition receptors that have been selected over evolutionary time to be highly pathogen-specific explains how the risks of autoreactivity in this system are minimized.

摘要

天然免疫系统的自我/非自我识别依赖于由天然免疫细胞表达的种系编码、无需重排的受体,这些受体识别保守的病原体相关分子模式。自然杀伤细胞2D(NKG2D)受体是一种强大的免疫激活受体,它结合人类基因组编码的配体,这些配体在正常组织中的表达可忽略不计,但在应激和疾病状态下会因尚不完全清楚的原因而增加。目前尚不清楚免疫系统如何协调自身蛋白的受体结合与自我/非自我识别以避免自身反应性。我们现在报告,病毒感染后NKG2D配体的表达增加取决于模式识别受体(RIG-I/MDA-5)检测到病毒双链RNA后激活的干扰素反应因子,并且NKG2D配体的上调可被病毒双链RNA结合蛋白的表达所阻断。因此,天然免疫介导的对病毒核酸的识别触发受感染细胞释放干扰素以募集自然杀伤细胞,并表达NKG2D配体,从而使其在免疫系统中更易被识别。最后,NKG2D配体诱导是模式识别受体信号传导的结果这一观察结果解释了该系统中自身反应性风险是如何在进化过程中被最小化的,因为这些模式识别受体经过选择具有高度的病原体特异性。