Inactivation of Target RNA Cleavage of a III-B CRISPR-Cas System Induces Robust Autoimmunity in Saccharolobus islandicus

Type III CRISPR-Cas systems show the target (tg)RNA-activated indiscriminate DNA cleavage and synthesis of oligoadenylates (cOA) and a secondary signal that activates downstream nuclease effectors to exert indiscriminate RNA/DNA cleavage, and both activities are regulated in a spatiotemporal fashion...

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Published in:International journal of molecular sciences 2022-07, Vol.23 (15), p.8515
Main Authors: Zhang, Yan, Lin, Jinzhong, Tian, Xuhui, Wang, Yuan, Zhao, Ruiliang, Wu, Chenwei, Wang, Xiaoning, Zhao, Pengpeng, Bi, Xiaonan, Yu, Zhenxiao, Han, Wenyuan, Peng, Nan, Liang, Yun Xiang, She, Qunxin
Format: Article
Language:English
Subjects:
Amino acids
Apoptosis
Autoimmunity
Autoimmunity - genetics
Cell death
Cleavage
Cmr4
CRISPR
CRISPR-Associated Proteins - genetics
CRISPR-Cas system
CRISPR-Cas Systems - genetics
Deoxyribonucleic acid
DNA
DNA biosynthesis
Dormancy
Effectors
Efficiency
Gene expression
Genes
Genomes
Immunization
Mutagenesis
Mutation
Nuclease
Plasmids
Proteins
Ribonuclease
RNA - genetics
RNA Cleavage
RNA-activated DNase
spatiotemporal regulation of Cmr systems
Sulfolobus - genetics
target RNA cleavage
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Summary:Type III CRISPR-Cas systems show the target (tg)RNA-activated indiscriminate DNA cleavage and synthesis of oligoadenylates (cOA) and a secondary signal that activates downstream nuclease effectors to exert indiscriminate RNA/DNA cleavage, and both activities are regulated in a spatiotemporal fashion. In III-B Cmr systems, cognate tgRNAs activate the two Cmr2-based activities, which are then inactivated via tgRNA cleavage by Cmr4, but how Cmr4 nuclease regulates the Cmr immunization remains to be experimentally characterized. Here, we conducted mutagenesis of Cmr4 conserved amino acids in , and this revealed that Cmr4α RNase-dead (dCmr4α) mutation yields cell dormancy/death. We also found that plasmid-borne expression of dCmr4α in the wild-type strain strongly reduced plasmid transformation efficiency, and deletion of CRISPR arrays in the host genome reversed the dCmr4α inhibition. Expression of dCmr4α also strongly inhibited plasmid transformation with Cmr2α and Cmr2α mutants, but the inhibition was diminished in Cmr2α . Since dCmr4α-containing effectors lack spatiotemporal regulation, this allows an everlasting interaction between crRNA and cellular RNAs to occur. As a result, some cellular RNAs, which are not effective in mediating immunity due to the presence of spatiotemporal regulation, trigger autoimmunity of the Cmr-α system in the cells expressing dCmr4α. Together, these results pinpoint the crucial importance of tgRNA cleavage in autoimmunity avoidance and in the regulation of immunization of type III systems.
ISSN:1422-0067
1661-6596
1422-0067
DOI:10.3390/ijms23158515