细胞生物学
DNA
胞浆
功能(生物学)
生物
先天免疫系统
C端
信号转导
生物化学
化学
酶
受体
氨基酸
作者
Jianli Tao,Xiaowei Zhang,Jianshi Jin,Xiaoxia Du,Tengfei Lian,Jing Yang,Xiang Zhou,Zhengfan Jiang,Xiao‐Dong Su
出处
期刊:Journal of Immunology
[American Association of Immunologists]
日期:2017-04-01
卷期号:198 (9): 3627-3636
被引量:80
标识
DOI:10.4049/jimmunol.1601909
摘要
Abstract The cytosolic DNA sensor cyclic GMP-AMP synthase (cGAS) mediates innate immune responses against invading pathogens, or against self-dsDNA, which causes autoimmune disorders. Upon nonspecific binding of cytosolic B–form DNA, cGAS synthesizes the second messenger 2′3′-cGAMP and triggers STING-dependent signaling to produce type I IFNs. The cGAS comprises less-conserved N-terminal residues and highly conserved nucleotidyltransferase/Mab21 domains. The function and structure of the well-conserved domains have been extensively studied, whereas the physiological function of the N-terminal domain of cGAS is largely uncharacterized. In this study we used a single-molecule technique combined with traditional biochemical and cellular assays to demonstrate that binding of nonspecific dsDNA by the N-terminal domain of cGAS promotes its activation. We have observed that the N terminus of human cGAS (hcGAS-N160) undergoes secondary structural change upon dsDNA binding in solution. Furthermore, we showed that the hcGAS-N160 helps full length hcGAS to expand the binding range on λDNA and facilitates its binding efficiency to dsDNA compared with hcGAS without the 160 N-terminal residues (hcGAS-d160). More importantly, hcGAS-N160 endows full length hcGAS relatively higher enzyme activity and stronger activation of STING/IRF3-mediated cytosolic DNA signaling. These findings strongly indicate that the N-terminal domain of cGAS plays an important role in enhancing its function.
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