先天免疫系统
坦克结合激酶1
生物
模式识别受体
组蛋白脱乙酰基酶
促炎细胞因子
串扰
表观遗传学
细胞生物学
信号转导
免疫学
组蛋白
激酶
免疫系统
炎症
蛋白激酶A
生物化学
MAP激酶激酶激酶
基因
物理
光学
作者
Xia Li,Qian Zhang,Yuanyuan Ding,Yiqi Liu,Dezhi Zhao,Kai Zhao,Qicong Shen,Xingguang Liu,Xuhui Zhu,Nan Li,Zhongyi Cheng,Guoping Fan,Qingqing Wang,Xuetao Cao
摘要
The DNA methyltransferase Dnmt3a has high expression in terminally differentiated macrophages; however, its role in innate immunity remains unknown. Here we report that deficiency in Dnmt3a selectively impaired the production of type I interferons triggered by pattern-recognition receptors (PRRs), but not that of the proinflammatory cytokines TNF and IL-6. Dnmt3a-deficient mice exhibited enhanced susceptibility to viral challenge. Dnmt3a did not directly regulate the transcription of genes encoding type I interferons; instead, it increased the production of type I interferons through an epigenetic mechanism by maintaining high expression of the histone deacetylase HDAC9. In turn, HDAC9 directly maintained the deacetylation status of the key PRR signaling molecule TBK1 and enhanced its kinase activity. Our data add mechanistic insight into the crosstalk between epigenetic modifications and post-translational modifications in the regulation of PRR signaling and activation of antiviral innate immune responses.
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