Modified tRNA anticodons are critical for proper mRNA translation during protein synthesis. It is generally thought that almost all bacterial tRNAs(Ile) use a modified cytidine-lysidine (L)-at the first position (34) of the anticodon to decipher the AUA codon as isoleucine (Ile). Here we report that tRNAs(Ile) from plant organelles and a subset of bacteria contain a new cytidine derivative, designated 2-aminovaleramididine (ava(2)C). Like L34, ava(2)C34 governs both Ile-charging ability and AUA decoding. Cryo-electron microscopy structural analyses revealed molecular details of codon recognition by ava(2)C34 with a specific interaction between its terminal amide group and an mRNA residue 3'-adjacent to the AUA codon. These findings reveal the evolutionary variation of an essential tRNA modification and demonstrate the molecular basis of AUA decoding mediated by a unique tRNA modification.
A tRNA modification with aminovaleramide facilitates AUA decoding in protein synthesis.
tRNA 与氨基戊酰胺的修饰促进了蛋白质合成中的 AUA 解码
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作者:Miyauchi Kenjyo, Kimura Satoshi, Akiyama Naho, Inoue Kazuki, Ishiguro Kensuke, Vu Thien-Son, Srisuknimit Veerasak, Koyama Kenta, Hayashi Gosuke, Soma Akiko, Nagao Asuteka, Shirouzu Mikako, Okamoto Akimitsu, Waldor Matthew K, Suzuki Tsutomu
| 期刊: | Nature Chemical Biology | 影响因子: | 13.700 |
| 时间: | 2025 | 起止号: | 2025 Apr;21(4):522-531 |
| doi: | 10.1038/s41589-024-01726-x | 研究方向: | 其它 |
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