AI Article Synopsis

  • - The study reveals that the RtcR CARF domain regulates two important RNA repair enzymes, RtcA and RtcB, which are necessary for activating transcription.
  • - RtcA and RtcB interact directly with RtcR, but while RtcAB’s catalytic activity is essential for transcription activation, it alone doesn’t suffice, suggesting another activating signal is required.
  • - This additional signal seems to come from the translation machinery, as RtcB repairs tmRNA, enhancing ribosome function and indicating CARF domain signaling has broader implications involving RNA repair and translation.

Article Abstract

CRISPR-associated Rossmann fold (CARF) domain signaling underpins modulation of CRISPR-Cas nucleases; however, the RtcR CARF domain controls expression of two conserved RNA repair enzymes, cyclase RtcA and ligase RtcB. Here, we demonstrate that RtcAB are required for RtcR-dependent transcription activation and directly bind to RtcR CARF. RtcAB catalytic activity is not required for complex formation with CARF, but is essential yet not sufficient for RtcRAB-dependent transcription activation, implying the need for an additional RNA repair-dependent activating signal. This signal differs from oligoadenylates, a known ligand of CARF domains, and instead appears to originate from the translation apparatus: RtcB repairs a tmRNA that rescues stalled ribosomes and increases translation elongation speed. Taken together, our data provide evidence for an expanded range for CARF domain signaling, including the first evidence of its control via protein-protein interactions, and a feed-forward mechanism to regulate RNA repair required for a functioning translation apparatus.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9650030PMC
http://dx.doi.org/10.1016/j.isci.2022.105425DOI Listing

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