Molecular basis of CD-NTase nucleotide selection in CBASS anti-phage defense
Öffentlich Deposited- Abstract
cGAS/DncV-like nucleotidyltransferase (CD-NTase) enzymes are signaling proteins that initiate antiviral immunity in animal cells and cyclic-oligonucleotide-based anti-phage signaling system (CBASS) phage defense in bacteria. Upon phage recognition, bacterial CD-NTases catalyze synthesis of cyclic-oligonucleotide signals, which activate downstream effectors and execute cell death. How CD-NTases control nucleotide selection to specifically induce defense remains poorly defined. Here, we combine structural and nucleotide-analog interference-mapping approaches to identify molecular rules controlling CD-NTase specificity. Structures of the cyclic trinucleotide synthase Enterobacter cloacae CdnD reveal coordinating nucleotide interactions and a possible role for inverted nucleobase positioning during product synthesis. We demonstrate that correct nucleotide selection in the CD-NTase donor pocket results in the formation of a thermostable-protein-nucleotide complex, and we extend our analysis to establish specific patterns governing selectivity for each of the major bacterial CD-NTase clades A–H. Our results explain CD-NTase specificity and enable predictions of nucleotide second-messenger signals within diverse antiviral systems.
- Creator
- Date Issued
- 2021
- Academic Affiliation
- Journal Title
- Journal Issue/Number
- 9
- Journal Volume
- 35
- Zuletzt geändert
- 2022-08-11
- Resource Type
- Urheberrechts-Erklärung
- License
- DOI
- ISSN
- 2211-1247
- Language
Beziehungen
Objekte
| Miniaturansicht | Titel | Hochladedatum | Sichtbarkeit | Aktionen |
|---|---|---|---|---|
|
|
1-s2.0-S2211124721005556-main.pdf | 2022-08-11 | Öffentlich | Herunterladen |