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. 2020 Jun;16(6):702-709.
doi: 10.1038/s41589-020-0500-6. Epub 2020 Mar 23.

An aminoacylation ribozyme evolved from a natural tRNA-sensing T-box riboswitch

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An aminoacylation ribozyme evolved from a natural tRNA-sensing T-box riboswitch

Satoshi Ishida et al. Nat Chem Biol. 2020 Jun.

Abstract

When the primitive translation system first emerged in the hypothetical RNA world, ribozymes could have been responsible for aminoacylation. Given that naturally occurring T-box riboswitches selectively sense the aminoacylation status of cognate tRNAs, we introduced a domain of random sequence into a T-box-tRNA conjugate and isolated ribozymes that were self-aminoacylating on the 3'-terminal hydroxyl group. One of them, named Tx2.1, recognizes the anticodon and D-loop of tRNA via interaction with its stem I domain, similarly to the parental T-box, and selectively charges N-biotinyl-L-phenylalanine (Bio-lPhe) onto the 3' end of the cognate tRNA in trans. We also demonstrated the ribosomal synthesis of a Bio-lPhe-initiated peptide in a Tx2.1-coupled in vitro translation system, in which Tx2.1 catalyzed specific tRNA aminoacylation in situ. This suggests that such ribozymes could have coevolved with a primitive translation system in the RNA world.

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