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Molecular basis of transcriptional repression of anti-CRISPR by anti-CRISPR-associated 2

Authors
Lee, So YeonKim, Gi EobPark, Hyun Ho
Issue Date
Jan-2022
Publisher
INT UNION CRYSTALLOGRAPHY
Keywords
Aca2; adaptive immunity; anti-CRISPR-associated 2; anti-CRISPR; CRISPR-Cas; Oceanimonas smirnovii; crystal structure
Citation
ACTA CRYSTALLOGRAPHICA SECTION D-STRUCTURAL BIOLOGY, v.78, pp 59 - 68
Pages
10
Journal Title
ACTA CRYSTALLOGRAPHICA SECTION D-STRUCTURAL BIOLOGY
Volume
78
Start Page
59
End Page
68
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/54598
DOI
10.1107/S2059798321011670
ISSN
2059-7983
Abstract
CRISPR-Cas systems are well known host defense mechanisms that are conserved in bacteria and archaea. To counteract CRISPR-Cas systems, phages and viruses have evolved to possess multiple anti-CRISPR (Acr) proteins that can inhibit the host CRISPR-Cas system via different strategies. The expression of acr genes is controlled by anti-CRISPR-associated (Aca) proteins that bind to an upstream promoter and regulate the expression of acr genes during transcription. Although the role of Aca as a transcriptional repressor has been demonstrated, the mechanism of action of Aca has not been determined. Here, the molecular mechanism underlying the Aca2-mediated transcriptional control of acr genes was elucidated by determining the crystal structure of Aca2 from Oceanimonas smirnovii at a high resolution of 1.92 angstrom. Aca2 forms a dimer in solution, and dimerization of Aca2 is critical for specific promoter binding. The promoter-binding strategy of dimeric Aca2 was also revealed by performing mutagenesis studies. The atomic structure of the Aca family shown in this study provides insights into the fine regulation of host defense and immune-escape mechanisms and also demonstrates the conserved working mechanism of the Aca family.
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