首页> 美国卫生研究院文献>Acta Crystallographica Section F: Structural Biology and Crystallization Communications >Structural mechanism of DNA recognition by the p202 HINa domain: insights into the inhibition of Aim2-mediated inflammatory signalling
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Structural mechanism of DNA recognition by the p202 HINa domain: insights into the inhibition of Aim2-mediated inflammatory signalling

机译:p202 HINa结构域识别DNA的结构机制:洞悉Aim2介导的炎症信号的抑制作用

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摘要

The HIN-200 family of proteins play significant roles in inflammation-related processes. Among them, AIM2 (absent in melanoma 2) and IFI16 (γ-interferon-inducible protein 16) recognize double-stranded DNA to initiate inflammatory responses. In contrast, p202, a mouse interferon-inducible protein containing two HIN domains (HINa and HINb), has been reported to inhibit Aim2-mediated inflammatory signalling in mouse. To understand the inhibitory mechanism, the crystal structure of the p202 HINa domain in complex with a 20 bp DNA was determined, in which p202 HINa nonspecifically recognizes both strands of DNA through electrostatic attraction. The p202 HINa domain binds DNA more tightly than does AIM2 HIN, and the DNA-binding mode of p202 HINa is different from that of the AIM2 HIN and IFI16 HINb domains. These results, together with the reported data on p202 HINb, lead to an interaction model for full-­length p202 and dsDNA which provides a conceivable mechanism for the negative regulation of Aim2 inflammasome activation by p202.
机译:HIN-200蛋白家族在炎症相关过程中起着重要作用。其中,AIM2(黑色素瘤2中不存在)和IFI16(γ-干扰素诱导蛋白16)识别双链DNA以启动炎症反应。相反,据报道,含有两个HIN域(HINa和HINb)的小鼠干扰素诱导蛋白p202可以抑制Aim2介导的小鼠炎症信号转导。为了理解抑制机理,确定了p202 HINa结构域与20bp DNA的复合物的晶体结构,其中p202 HINa通过静电吸引非特异性地识别DNA的两条链。与AIM2 HIN相比,p202 HINa结构域与DNA的结合更紧密,而p202 HINa的DNA结合模式与AIM2 HIN和IFI16 HINb结构域的结合模式不同。这些结果,加上有关p202 HINb的报道数据,导致了全长p202和dsDNA的相互作用模型,为p202对Aim2炎性体激活的负调控提供了可能的机制。

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