特里夫
TLR3型
干扰素
内部收益率3
先天免疫系统
信号转导
细胞生物学
Toll样受体
生物
病毒学
免疫系统
免疫学
作者
Yisha Liang,Xuezhi Cao,Qiang Ding,Yanan Zhao,Zhenliang He,Jin Zhong
出处
期刊:PLOS Pathogens
[Public Library of Science]
日期:2018-05-21
卷期号:14 (5): e1007075-e1007075
被引量:36
标识
DOI:10.1371/journal.ppat.1007075
摘要
Toll-like receptor 3 (TLR3) senses dsRNA intermediates produced during RNA virus replication to activate innate immune signaling pathways through adaptor protein TRIF. Many viruses have evolved strategies to block TLR3-mediated interferon signaling via targeting TRIF. Here we studied how hepatitis C virus (HCV) antagonizes the TLR3-mediated interferon signaling. We found that HCV-encoded NS4B protein inhibited TLR3-mediated interferon signaling by down-regulating TRIF protein level. Mechanism studies indicated that the downregulation of TRIF by NS4B was dependent on caspase8. NS4B transfection or HCV infection can activate caspase8 to promote TRIF degradation, leading to suppression of TLR3-mediated interferon signaling. Knockout of caspase8 can prevent TRIF degradation triggered by NS4B, thereby enhancing the TLR3-mediated interferon signaling activation in response to HCV infection. In conclusion, our work revealed a new mechanism for HCV to evade innate immune response by blocking the TLR3-mediated interferon signaling via NS4B-induced TRIF degradation.
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