猪IKKε参与STING诱导的胞质DNA信号通路的I型IFN抗病毒反应。

The Journal of Biological Chemistry Pub Date : 2023-10-01 Epub Date: 2023-09-01 DOI:10.1016/j.jbc.2023.105213
Jia Luo, Qi Cao, Jiajia Zhang, Sen Jiang, Nengwen Xia, Shaohua Sun, Wanglong Zheng, Nanhua Chen, Francois Meurens, Jianzhong Zhu
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引用次数: 0

摘要

环状GMP-AMP合酶和干扰素(IFN)基因刺激因子(cGAS-STING)途径是先天免疫防御的关键组成部分,并通过诱导I型IFN的表达发挥巨大的抗病毒活性。目前,STING激活的I型IFN的产生被认为仅由TANK结合激酶1(TBK1)介导。在这里,我们发现猪IKKε(pIKKε)也直接参与STING诱导的I型IFN表达和使用IKKε-/-猪巨噬细胞的抗病毒反应。与pTBK1类似,pIKKε与C末端尾部的pSTING直接相互作用。此外,pSTING C末端尾部的TBK1结合基序对于其与pIKKε的相互作用是必需的,并且在TBK1结合基序中,亮氨酸(L)373对于相互作用也是关键的。另一方面,pIKKε的激酶结构域和支架二聚化结构域都参与了与pSTING的相互作用。一致地,pKKε及其突变体在IKKε-/-猪巨噬细胞中的重建证实了IKKε及其激酶结构域和支架二聚化结构域都参与STING信号传导和抗病毒功能。因此,我们的发现加深了对猪cGAS-STING通路的理解,为有效的抗病毒治疗猪病毒性疾病奠定了基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Porcine IKKε is involved in the STING-induced type I IFN antiviral response of the cytosolic DNA signaling pathway.

Porcine IKKε is involved in the STING-induced type I IFN antiviral response of the cytosolic DNA signaling pathway.

Porcine IKKε is involved in the STING-induced type I IFN antiviral response of the cytosolic DNA signaling pathway.

Porcine IKKε is involved in the STING-induced type I IFN antiviral response of the cytosolic DNA signaling pathway.

The cyclic GMP-AMP synthase and stimulator of interferon (IFN) genes (cGAS-STING) pathway serves as a crucial component of innate immune defense and exerts immense antiviral activity by inducing the expression of type I IFNs. Currently, STING-activated production of type I IFNs has been thought to be mediated only by TANK-binding kinase 1 (TBK1). Here, we identified that porcine IKKε (pIKKε) is also directly involved in STING-induced type I IFN expression and antiviral response by using IKKε-/- porcine macrophages. Similar to pTBK1, pIKKε interacts directly with pSTING on the C-terminal tail. Furthermore, the TBK1-binding motif of pSTING C-terminal tail is essential for its interaction with pIKKε, and within the TBK1-binding motif, the leucine (L) 373 is also critical for the interaction. On the other hand, both kinase domain and scaffold dimerization domain of pIKKε participate in the interactions with pSTING. Consistently, the reconstitution of pIKKε and its mutants in IKKε-/- porcine macrophages corroborated that IKKε and its kinase domain and scaffold dimerization domain are all involved in the STING signaling and antiviral function. Thus, our findings deepen the understanding of porcine cGAS-STING pathway, which lays a foundation for effective antiviral therapeutics against porcine viral diseases.

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