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

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作者
Satoshi Ishida
Naohiro Terasaka
Takayuki Katoh
Hiroaki Suga
机构
[1] The University of Tokyo,Department of Chemistry, Graduate School of Science
来源
Nature Chemical Biology | 2020年 / 16卷
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摘要
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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页码:702 / 709
页数:7
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