单个噬菌体蛋白可封存来自 TIR 和 cGAS 类酶的信号

IF 3.7 2区 化学 Q2 CHEMISTRY, MULTIDISCIPLINARY Langmuir Pub Date : 2024-10-30 DOI:10.1038/s41586-024-08122-4
Dong Li, Yu Xiao, Iana Fedorova, Weijia Xiong, Yu Wang, Xi Liu, Erin Huiting, Jie Ren, Zirui Gao, Xingyu Zhao, Xueli Cao, Yi Zhang, Joseph Bondy-Denomy, Yue Feng
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引用次数: 0

摘要

原核生物抗噬菌体免疫系统利用 TIR 和 cGAS 类酶产生 1′′-3′-glycocyclic ADP-ribose (1′′-3′-gcADPR)和环状二核苷酸(CDN)及环状三核苷酸(CTN)信号分子,分别限制噬菌体的复制1,2,3。然而,噬菌体如何中和这些不同的共同系统在很大程度上还不清楚。在这里,我们发现 Thoeris 抗防御蛋白 Tad14 和 Tad25 都能通过同时封存 CBASS 环状寡核苷酸来实现抗环状寡核苷酸抗噬菌体信号系统(anti-CBASS)的活性。除了与 Thoeris 信号 1′′-3′-gcADPR 和 1′′-2′-gcADPR 结合外,Tad1 还以高亲和力与许多 CBASS CDN 和 CTN 结合,抑制在体内和体外使用这些分子的 CBASS 系统。六聚体 Tad1 有六个与 CDN 或 gcADPR 结合的位点,它们与 CTN 的两个高亲和力结合位点无关。Tad2 形成一个四聚体,除了 gcADPR 分子外,它还能封存各种 CDN,利用不同的结合位点同时与这些信号结合。因此,Tad1 和 Tad2 都是双管齐下的抑制剂,它们与抗 CBASS 蛋白 2(Acb26,7,8)一起,确立了噬菌体蛋白利用不同结合位点灵活封存大量环核苷酸的范例。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Single phage proteins sequester signals from TIR and cGAS-like enzymes

Prokaryotic anti-phage immune systems use TIR and cGAS-like enzymes to produce 1′′-3′-glycocyclic ADP-ribose (1′′-3′-gcADPR) and cyclic dinucleotide (CDN) and cyclic trinucleotide (CTN) signalling molecules, respectively, which limit phage replication1,2,3. However, how phages neutralize these distinct and common systems is largely unclear. Here we show that the Thoeris anti-defence proteins Tad14 and Tad25 both achieve anti-cyclic-oligonucleotide-based anti-phage signalling system (anti-CBASS) activity by simultaneously sequestering CBASS cyclic oligonucleotides. Apart from binding to the Thoeris signals 1′′-3′-gcADPR and 1′′-2′-gcADPR, Tad1 also binds to numerous CBASS CDNs and CTNs with high affinity, inhibiting CBASS systems that use these molecules in vivo and in vitro. The hexameric Tad1 has six binding sites for CDNs or gcADPR, which are independent of the two high-affinity binding sites for CTNs. Tad2 forms a tetramer that also sequesters various CDNs in addition to gcADPR molecules, using distinct binding sites to simultaneously bind to these signals. Thus, Tad1 and Tad2 are both two-pronged inhibitors that, alongside anti-CBASS protein 2 (Acb26,7,8), establish a paradigm of phage proteins that use distinct binding sites to flexibly sequester a considerable breadth of cyclic nucleotides.

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来源期刊
Langmuir
Langmuir 化学-材料科学:综合
CiteScore
6.50
自引率
10.30%
发文量
1464
审稿时长
2.1 months
期刊介绍: Langmuir is an interdisciplinary journal publishing articles in the following subject categories: Colloids: surfactants and self-assembly, dispersions, emulsions, foams Interfaces: adsorption, reactions, films, forces Biological Interfaces: biocolloids, biomolecular and biomimetic materials Materials: nano- and mesostructured materials, polymers, gels, liquid crystals Electrochemistry: interfacial charge transfer, charge transport, electrocatalysis, electrokinetic phenomena, bioelectrochemistry Devices and Applications: sensors, fluidics, patterning, catalysis, photonic crystals However, when high-impact, original work is submitted that does not fit within the above categories, decisions to accept or decline such papers will be based on one criteria: What Would Irving Do? Langmuir ranks #2 in citations out of 136 journals in the category of Physical Chemistry with 113,157 total citations. The journal received an Impact Factor of 4.384*. This journal is also indexed in the categories of Materials Science (ranked #1) and Multidisciplinary Chemistry (ranked #5).
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