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RNA 和咪唑并喹啉啉通过不同的 TLR7/8 胞外结构域被感知,导致功能不同的信号事件。

RNA and imidazoquinolines are sensed by distinct TLR7/8 ectodomain sites resulting in functionally disparate signaling events.

机构信息

Junior Research Group Toll-Like Receptors and Cancer, German Cancer Research Center, 69120 Heidelberg, Germany;

Weatherall Institute of Molecular Medicine, University of Oxford, Oxford OX3 9DS, United Kingdom;

出版信息

J Immunol. 2014 Jun 15;192(12):5963-73. doi: 10.4049/jimmunol.1303058. Epub 2014 May 9.

DOI:10.4049/jimmunol.1303058
PMID:24813206
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4066583/
Abstract

TLRs 7 and 8 are pattern recognition receptors controlling antiviral host defense or autoimmune diseases. Apart from foreign and host RNA, synthetic RNA oligoribonucleotides (ORN) or small molecules of the imidazoquinoline family activate TLR7 and 8 and are being developed as therapeutic agonists. The structure-function relationships for RNA ORN and imidazoquinoline sensing and consequent downstream signaling by human TLR7 and TLR8 are unknown. Proteome- and genome-wide analyses in primary human monocyte-derived dendritic cells here showed that TLR8 sensing of RNA ORN versus imidazoquinoline translates to ligand-specific differential phosphorylation and transcriptional events. In addition, TLR7 and 8 ectodomains were found to discriminate between RNA ORN and imidazoquinolines by overlapping and nonoverlapping recognition sites to which murine loss-of-function mutations and human naturally occurring hyporesponsive polymorphisms map. Our data suggest TLR7 and TLR8 can signal in two different "modes" depending on the class of ligand. Considering RNA ORN and imidazoquinolines have been regarded as functionally interchangeable, our study highlights important functional incongruities whose understanding will be important for developing TLR7 or 8 therapeutics with desirable effector and safety profiles for in vivo application.

摘要

TLRs 7 和 8 是识别受体,控制抗病毒宿主防御或自身免疫性疾病。除了外来和宿主 RNA 外,合成的 RNA 寡核糖核苷酸(ORN)或咪唑并喹啉家族的小分子激活 TLR7 和 8,并被开发为治疗性激动剂。人类 TLR7 和 TLR8 对 RNA ORN 和咪唑并喹啉的感知以及随之而来的下游信号传导的结构 - 功能关系尚不清楚。这里对原代人单核细胞衍生的树突状细胞进行的蛋白质组和基因组分析表明,RNA ORN 与咪唑并喹啉对 TLR8 的感应转化为配体特异性的差异磷酸化和转录事件。此外,TLR7 和 8 的细胞外结构域被发现通过重叠和非重叠的识别位点来区分 RNA ORN 和咪唑并喹啉,这些识别位点映射到鼠功能丧失突变和人类天然低反应性多态性。我们的数据表明,TLR7 和 TLR8 可以根据配体的类别以两种不同的“模式”发出信号。鉴于 RNA ORN 和咪唑并喹啉被认为在功能上可互换,我们的研究强调了重要的功能不一致性,了解这些功能不一致性对于开发具有理想效应和安全性的 TLR7 或 8 治疗药物以用于体内应用非常重要。

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