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Crystal structure of the ubiquitin-like domain of human TBK1

机译:人TBK1泛素样结构域的晶体结构

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TANK-binding kinase 1 (TBK1) is an important enzyme in the regulation of cellular antiviral effects. TBK1 regulates the activity of the interferon regulatory factors IRF3 and IRF7, thereby playing a key role in type I interferon (IFN) signaling pathways. The structure of TBK1 consists of an N-terminal kinase domain, a middle ubiquitin-like domain (ULD), and a C-terminal elongated helical domain. It has been reported that the ULD of TBK1 regulates kinase activity, playing an important role in signaling and mediating interactions with other molecules in the IFN pathway. In this study, we present the crystal structure of the ULD of human TBK1 and identify several conserved residues by multiple sequence alignment. We found that a hydrophobic patch in TBK1, containing residues Leu316, Ile353, and Val382, corresponding to the “Ile44 hydrophobic patch” observed in ubiquitin, was conserved in TBK1, IκB kinase epsilon (IKK?/IKKi), IκB kinase alpha (IKKα), and IκB kinase beta (IKKβ). In comparison with the structure of the IKKβ ULD domain of Xenopus laevis , we speculate that the Ile44 hydrophobic patch of TBK1 is present in an intramolecular binding surface between ULD and the C-terminal elongated helices. The varying surface charge distributions in the ULD domains of IKK and IKK-related kinases may be relevant to their specificity for specific partners.
机译:TANK结合激酶1(TBK1)是调节细胞抗病毒作用的重要酶。 TBK1调节干扰素调节因子IRF3和IRF7的活性,从而在I型干扰素(IFN)信号传导途径中发挥关键作用。 TBK1的结构由N端激酶结构域,中间泛素样结构域(ULD)和C端细长螺旋结构域组成。据报道,TBK1的ULD调节激酶活性,在信号传导和介导与IFN途径中其他分子的相互作用中起重要作用。在这项研究中,我们介绍了人TBK1 ULD的晶体结构,并通过多重序列比对鉴定了几个保守残基。我们发现在TBK1,IκB激酶epsilon(IKK?/ IKKi),IκB激酶α(IKKα)中保守了TBK1中的疏水补丁,其中包含残基Leu316,Ile353和Val382,与遍在蛋白中观察到的“ Ile44疏水补丁”相对应。 )和IκB激酶beta(IKKβ)。与非洲爪蟾的IKKβULD结构域的结构相比,我们推测TBK1的Ile44疏水膜存在于ULD和C端细长螺旋之间的分子内结合表面。 IKK和IKK相关激酶的ULD结构域中表面电荷分布的变化可能与其对特定伴侣的特异性有关。

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