STING cyclic dinucleotide sensing originated in bacteria

干扰素基因刺激剂 效应器 先天免疫系统 细胞生物学 生物 遗传学 受体 工程类 航空航天工程
作者
Benjamin R. Morehouse,Apurva A. Govande,Adi Millman,Alexander F. A. Keszei,B. Lowey,Gal Ofir,Sichen Shao,Rotem Sorek,Philip J. Kranzusch
出处
期刊:Nature [Nature Portfolio]
卷期号:586 (7829): 429-433 被引量:390
标识
DOI:10.1038/s41586-020-2719-5
摘要

Stimulator of interferon genes (STING) is a receptor in human cells that senses foreign cyclic dinucleotides that are released during bacterial infection and in endogenous cyclic GMP-AMP signalling during viral infection and anti-tumour immunity1-5. STING shares no structural homology with other known signalling proteins6-9, which has limited attempts at functional analysis and prevented explanation of the origin of cyclic dinucleotide signalling in mammalian innate immunity. Here we reveal functional STING homologues encoded within prokaryotic defence islands, as well as a conserved mechanism of signal activation. Crystal structures of bacterial STING define a minimal homodimeric scaffold that selectively responds to cyclic di-GMP synthesized by a neighbouring cGAS/DncV-like nucleotidyltransferase (CD-NTase) enzyme. Bacterial STING domains couple the recognition of cyclic dinucleotides with the formation of protein filaments to drive oligomerization of TIR effector domains and rapid NAD+ cleavage. We reconstruct the evolutionary events that followed the acquisition of STING into metazoan innate immunity, and determine the structure of a full-length TIR-STING fusion from the Pacific oyster Crassostrea gigas. Comparative structural analysis demonstrates how metazoan-specific additions to the core STING scaffold enabled a switch from direct effector function to regulation of antiviral transcription. Together, our results explain the mechanism of STING-dependent signalling and reveal the conservation of a functional cGAS-STING pathway in prokaryotic defence against bacteriophages.
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