Journal
NATURE COMMUNICATIONS
Volume 12, Issue 1, Pages -Publisher
NATURE PORTFOLIO
DOI: 10.1038/s41467-021-24076-x
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Funding
- Deutsche Forschungsgemeinschaft [IG73/14-2, WI2381/6-1, INST 152/775-1 FUGG]
- Swedish Research Council [2016-06264, 2018-05946, 2018-05498]
- University of Hamburg
- Swedish Research Council [2018-05946, 2018-05498] Funding Source: Swedish Research Council
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The researchers designed novel tRNAs that decode UGA stop codons in E. coli efficiently by optimizing the tRNA structure to enhance suppression activity. The study determined the ribosome structure bound to the designed tRNA with a UGA stop codon, showing that the conformation of the stop codon is influenced by distinct A-site ligands.
Three stop codons (UAA, UAG and UGA) terminate protein synthesis and are almost exclusively recognized by release factors. Here, we design de novo transfer RNAs (tRNAs) that efficiently decode UGA stop codons in Escherichia coli. The tRNA designs harness various functionally conserved aspects of sense-codon decoding tRNAs. Optimization within the T Psi C-stem to stabilize binding to the elongation factor, displays the most potent effect in enhancing suppression activity. We determine the structure of the ribosome in a complex with the designed tRNA bound to a UGA stop codon in the A site at 2.9 angstrom resolution. In the context of the suppressor tRNA, the conformation of the UGA codon resembles that of a sense-codon rather than when canonical translation termination release factors are bound, suggesting conformational flexibility of the stop codons dependent on the nature of the A-site ligand. The systematic analysis, combined with structural insights, provides a rationale for targeted repurposing of tRNAs to correct devastating nonsense mutations that introduce a premature stop codon. Here, the authors report de novo design, optimization and characterization of tRNAs that decode UGA stop codons in E. coli. The structure of the ribosome in a complex with the designed tRNA bound to a UGA stop codon suggests that distinct A-site ligands (tRNAs versus release factors) induce distinct conformation of the stop codon within the mRNA in the decoding center.
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