生物
毒力
粘液瘤病毒
病菌
病毒学
免疫系统
免疫
病毒
干扰素
先天免疫系统
功能(生物学)
核糖核酸
病毒复制
锌指
信号转导
RNA干扰
第一行
人类病原体
干扰素调节因子
细胞培养
免疫学
单核细胞
细胞生物学
机制(生物学)
防御机制
遗传学
毒力因子
作者
Brenna C. Remick,Junhao Mao,Andrew G. Manford,Ami D. Gutierrez-Jensen,Allon Wagner,Michael Rapé,Grant McFadden,Mursheda Rahman,Moritz M. Gaidt,Daniel E. Zak
出处
期刊:Science
[American Association for the Advancement of Science]
日期:2026-02-12
卷期号:391 (6786): eadw4937-eadw4937
标识
DOI:10.1126/science.adw4937
摘要
Effector-triggered immunity (ETI) is a form of pathogen sensing that involves detection of pathogen-encoded virulence factors or "effectors." To discover ETI pathways in mammals, we developed a screening approach in which we expressed individual virulence factors in a human monocyte cell line and assessed transcriptional responses by RNA sequencing. We identified a poxvirus effector, myxoma virus M3.1, which elicited an antiviral nuclear factor κB (NF-κB) response. NF-κB was unleashed by an ETI pathway that sensed M3.1 attack of two antiviral complexes: zinc finger antiviral protein and TBK1. NF-κΒ activation occurred because the proteins inhibited by M3.1-N4BP1, ZC3H12A, and TBK1-are negative regulators of NF-κB. Our study established a systematic approach for the discovery of ETI pathways, and the results illustrated how negative regulators of immune responses may function in pathogen sensing.
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