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


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.

SUBMITTER: Lim CS 

PROVIDER: S-EPMC9653405 | biostudies-literature | 2022 Nov

REPOSITORIES: biostudies-literature

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

Lim Chan Seok CS   Jang Yoon Ha YH   Lee Ga Young GY   Han Gu Min GM   Jeong Hye Jin HJ   Kim Ji Won JW   Lee Jie-Oh JO  

Nature communications 20221112 1


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 le  ...[more]

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