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关键免疫蛋白 TRAF6 和 TIFA 之间的结合和增强结合。

Binding and Enhanced Binding between Key Immunity Proteins TRAF6 and TIFA.

机构信息

Institute of Biological Chemistry, Academia Sinica, 128 Academia Road Sec. 2, Nankang, Taipei, 115, Taiwan.

Institute of Biochemical Sciences, National (Taiwan) University, 1, Roosevelt Road Sec. 4, Taipei, 106, Taiwan.

出版信息

Chembiochem. 2019 Jan 18;20(2):140-146. doi: 10.1002/cbic.201800436. Epub 2018 Dec 13.

Abstract

Human tumor necrosis factor receptor associated factor (TRAF)-interacting protein, with a forkhead-associated domain (TIFA), is a key regulator of NF-κB activation. It also plays a key role in the activation of innate immunity in response to bacterial infection, through heptose 1,7-bisphosphate (HBP); a metabolite of lipopolysaccharide (LPS). However, the mechanism of TIFA function is largely unexplored, except for the suggestion of interaction with TRAF6. Herein, we provide evidence for direct binding, albeit weak, between TIFA and the TRAF domain of TRAF6, and it is shown that the binding is enhanced for a rationally designed double mutant, TIFA S174Q/M179D. Enhanced binding was also demonstrated for endogenous full-length TRAF6. Furthermore, the structures of the TRAF domain complexes with the consensus TRAF-binding peptides from the C terminus of wild-type and S174Q/M179D mutant TIFA, showing salt-bridge formation between residues 177-181 of TIFA and the binding pocket residues of the TRAF domain, were solved. Taken together, the results provide direct evidence and a structural basis for the TIFA-TRAF6 interaction, and show how this important biological function can be modulated.

摘要

人肿瘤坏死因子受体相关因子(TRAF)相互作用蛋白,具有一个与叉头相关的结构域(TIFA),是 NF-κB 激活的关键调节因子。它还在细菌感染引起的固有免疫激活中发挥关键作用,通过庚糖 1,7-双磷酸(HBP);脂多糖(LPS)的代谢物。然而,TIFA 功能的机制在很大程度上尚未被探索,除了与 TRAF6 相互作用的建议。本文提供了 TIFA 与 TRAF6 的 TRAF 结构域之间直接结合的证据,尽管结合较弱,但对于合理设计的双突变体 TIFA S174Q/M179D,显示出结合增强。内源性全长 TRAF6 的结合也得到了增强。此外,还解决了 TRAF 结构域与野生型和 S174Q/M179D 突变型 TIFA C 末端的保守 TRAF 结合肽的复合物的结构,显示 TIFA 的残基 177-181 与 TRAF 结构域的结合口袋残基之间形成盐桥。总之,这些结果为 TIFA-TRAF6 相互作用提供了直接证据和结构基础,并展示了如何调节这种重要的生物学功能。

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