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[Toll样受体感知单链核酸的结构分析及其应用]

[Structural Analyses of Toll-like Receptor Sensing Single-stranded Nucleic Acids and Its Application].

作者信息

Shimizu Toshiyuki

机构信息

Graduate School of Pharmaceutical Sciences, The University of Tokyo.

出版信息

Yakugaku Zasshi. 2016;136(2):173-8. doi: 10.1248/yakushi.15-00229-1.

Abstract

Toll-like receptors (TLRs) are a family of pattern-recognition receptors that recognize microbial components and initiate subsequent immune responses. TLR7 and TLR8 recognize single-stranded (ss)RNA and initiate innate immune responses. Moreover, several small-molecule compounds have been identified as TLR7 and TLR8 activators. We determined the crystal structures of unliganded and ligand-induced activated human TLR8 dimers. Upon ligand stimulation, the TLR8 dimer was reorganized such that the two C-termini were brought into proximity. Ligand binding induces reorganization of the TLR8 dimer, which enables downstream signaling processes. To elucidate how TLR8 recognizes its natural ligand, ssRNA, as well as how the receptor can be activated by ssRNA that is structurally and chemically very different from the chemical ligands, we performed crystallographic studies of TLR8 in complex with ssRNA. TLR8 recognizes, at distinct sites, uridine and small oligonucleotides derived from the degradation of ssRNA. Uridine bound the site on the dimerization interface where small chemical ligands are recognized, whereas short oligonucleotides bound a newly identified site. Based on structural information, new compounds have been developed. We describe the crystal structure of a newly developed agonist, C2-butyl furo[2,3-c]quinolone.

摘要

Toll样受体(TLRs)是一类模式识别受体,可识别微生物成分并引发后续免疫反应。TLR7和TLR8识别单链(ss)RNA并引发先天性免疫反应。此外,几种小分子化合物已被鉴定为TLR7和TLR8激活剂。我们确定了未结合配体和配体诱导激活的人TLR8二聚体的晶体结构。在配体刺激下,TLR8二聚体重组,使两个C末端靠近。配体结合诱导TLR8二聚体重组,从而启动下游信号传导过程。为了阐明TLR8如何识别其天然配体ssRNA,以及该受体如何被结构和化学性质与化学配体非常不同的ssRNA激活,我们进行了TLR8与ssRNA复合物的晶体学研究。TLR8在不同位点识别尿苷和源自ssRNA降解的小寡核苷酸。尿苷结合二聚化界面上识别小化学配体的位点,而短寡核苷酸结合新鉴定的位点。基于结构信息,已开发出新化合物。我们描述了一种新开发的激动剂C2-丁基呋喃并[2,3-c]喹诺酮的晶体结构。

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