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  5. tRNA anticodon cleavage by target-activated CRISPR-Cas13a effector

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Article
en
2024

tRNA anticodon cleavage by target-activated CRISPR-Cas13a effector

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en
2024
Vol 10 (17)
Vol. 10
DOI: 10.1126/sciadv.adl0164

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Eugene V Koonin
Eugene V Koonin

National Center for Biotechnology Information

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Ishita Jain
Matvey Kolesnik
Konstantin Kuznedelov
+12 more

Abstract

Type VI CRISPR-Cas systems are among the few CRISPR varieties that target exclusively RNA. The CRISPR RNA–guided, sequence-specific binding of target RNAs, such as phage transcripts, activates the type VI effector, Cas13. Once activated, Cas13 causes collateral RNA cleavage, which induces bacterial cell dormancy, thus protecting the host population from the phage spread. We show here that the principal form of collateral RNA degradation elicited by Leptotrichia shahii Cas13a expressed in Escherichia coli cells is the cleavage of anticodons in a subset of transfer RNAs (tRNAs) with uridine-rich anticodons. This tRNA cleavage is accompanied by inhibition of protein synthesis, thus providing defense from the phages. In addition, Cas13a-mediated tRNA cleavage indirectly activates the RNases of bacterial toxin-antitoxin modules cleaving messenger RNA, which could provide a backup defense. The mechanism of Cas13a-induced antiphage defense resembles that of bacterial anticodon nucleases, which is compatible with the hypothesis that type VI effectors evolved from an abortive infection module encompassing an anticodon nuclease.

How to cite this publication

Ishita Jain, Matvey Kolesnik, Konstantin Kuznedelov, Leonid Minakhin, Natalia Morozova, Anna Shiriaeva, Alexandr Kirillov, Sofia Medvedeva, Alexei Livenskyi, L.Sh. Kazieva, Kira S. Makarova, Eugene V Koonin, Sergei Borukhov, Konstantin Severinov, Ekaterina Semenova (2024). tRNA anticodon cleavage by target-activated CRISPR-Cas13a effector. , 10(17), DOI: https://doi.org/10.1126/sciadv.adl0164.

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Publication Details

Type

Article

Year

2024

Authors

15

Datasets

0

Total Files

0

Language

en

DOI

https://doi.org/10.1126/sciadv.adl0164

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