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与DMXAA复合的小鼠STING 54 kDa二聚体C端结构域的主链共振归属

Backbone resonance assignments of the 54 kDa dimeric C-terminal domain of murine STING in complex with DMXAA.

作者信息

Lou Yuan-Chao, Kao Yi-Fen, Chin Ko-Hsin, Chen Jen-Kang, Tu Je-Le, Chen Chinpan, Chou Shan-Ho

机构信息

Institute of Biomedical Sciences, Academia Sinica, Taipei, 115, Taiwan, ROC.

Agricultural Biotechnology Center, National Chung Hsing University, Taichung, 40227, Taiwan, ROC.

出版信息

Biomol NMR Assign. 2015 Oct;9(2):271-4. doi: 10.1007/s12104-014-9590-y. Epub 2014 Dec 9.

Abstract

The mammalian ER protein STING (stimulators of interferon genes) is an important innate immunity protein for linking detection of novel secondary messengers c-di-GMP, c-di-AMP, cGAMP or cytosolic dsDNA to the activation of TANK kinase 1 and its downstream interferon regulator factor 3. Recently quite a few of crystal structures representing different states of the C-terminal domain (CTD) of human and murine STING (hSTING and mSTING) in complex with c-di-GMP, cGAMP or DMXAA have been reported. However, the C-terminal 42 residues of STING-CTD, which may be important in mediating the downstream reactions, is invisible or absent in all reported X-ray structures. In addition, X-ray crystal structures may be subject to crystal packing force. Hence an alternate method of determining the structure and function of STING in a near physiological condition is essential. We now report the near complete backbone resonance assignments of the 54 kDa dimeric mSTING-CTD in complex with DMXAA, which is the first step in determining its complex structure and understanding why DMXAA, which is a very efficient agent for curing mouse cancer, is totally ineffective in human.

摘要

哺乳动物内质网蛋白STING(干扰素基因刺激因子)是一种重要的天然免疫蛋白,可将新型第二信使c-di-GMP、c-di-AMP、cGAMP或胞质双链DNA的检测与TANK激酶1及其下游干扰素调节因子3的激活联系起来。最近,已经报道了一些代表人类和小鼠STING(hSTING和mSTING)C末端结构域(CTD)与c-di-GMP、cGAMP或DMXAA结合的不同状态的晶体结构。然而,STING-CTD的C末端42个残基在所有已报道的X射线结构中均不可见或缺失,而这些残基可能在介导下游反应中起重要作用。此外,X射线晶体结构可能受到晶体堆积力的影响。因此,在接近生理条件下确定STING结构和功能的另一种方法至关重要。我们现在报告与DMXAA结合的54 kDa二聚体mSTING-CTD的近乎完整的主链共振归属,这是确定其复杂结构以及理解为什么DMXAA(一种对治疗小鼠癌症非常有效的药物)对人类完全无效的第一步。

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