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TLR3 与聚(I:C)RNA 配体结合时形成高度有序的簇。

TLR3 forms a highly organized cluster when bound to a poly(I:C) RNA ligand.

机构信息

Department of Life Sciences and POSTECH, Pohang, 37673, Korea.

Institute of Membrane Proteins, POSTECH, Pohang, 37673, Korea.

出版信息

Nat Commun. 2022 Nov 12;13(1):6876. doi: 10.1038/s41467-022-34602-0.

Abstract

Toll-like Receptor 3 (TLR3) initiates a potent anti-viral immune response by binding to double-stranded RNA ligands. Previous crystallographic studies showed that TLR3 forms a homodimer when bound to a 46-base pair RNA ligand. However, this short RNA fails to initiate a robust immune response. To obtain structural insights into the length dependency of TLR3 ligands, we determine the cryo-electron microscopy structure of full-length TLR3 in a complex with a synthetic RNA ligand with an average length of ~400 base pairs. In the structure, the dimeric TLR3 units are clustered along the double-stranded RNA helix in a highly organized and cooperative fashion with a uniform inter-dimer spacing of 103 angstroms. The intracellular and transmembrane domains are dispensable for the clustering because their deletion does not interfere with the cluster formation. Our structural observation suggests that ligand-induced clustering of TLR3 dimers triggers the ordered assembly of intracellular signaling adaptors and initiates a robust innate immune response.

摘要

Toll 样受体 3(TLR3)通过与双链 RNA 配体结合,启动有效的抗病毒免疫反应。先前的晶体学研究表明,TLR3 与 46 个碱基对的 RNA 配体结合时形成同源二聚体。然而,这种短的 RNA 并不能引发强烈的免疫反应。为了深入了解 TLR3 配体的长度依赖性,我们通过冷冻电镜技术确定了全长 TLR3 与平均长度约为 400 个碱基对的合成 RNA 配体形成复合物的结构。在该结构中,二聚体 TLR3 单元以高度有序和协作的方式沿着双链 RNA 螺旋聚集,两个二聚体之间的间隔均匀,为 103 埃。细胞内和跨膜结构域对于聚集是可有可无的,因为它们的缺失并不干扰聚集的形成。我们的结构观察表明,配体诱导的 TLR3 二聚体聚集触发了细胞内信号转导衔接蛋白的有序组装,并引发了强烈的先天免疫反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5dd9/9653405/578b9c593b11/41467_2022_34602_Fig1_HTML.jpg

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