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Structural insights into mRNA reading frame regulation by tRNA modification and slippery codon–anticodon pairing

Eric D. Hoffer, Samuel Hong, S. Sunita, Tatsuya Maehigashi, Ruben L. Gonzalez, Paul C. Whitford, C.M. Dunham

2020eLife43 citationsDOIOpen Access PDF

Abstract

Modifications in the tRNA anticodon loop, adjacent to the three-nucleotide anticodon, influence translation fidelity by stabilizing the tRNA to allow for accurate reading of the mRNA genetic code. One example is the N1-methylguanosine modification at guanine nucleotide 37 (m 1 G37) located in the anticodon loop andimmediately adjacent to the anticodon nucleotides 34, 35, 36. The absence of m 1 G37 in tRNA Pro causes +1 frameshifting on polynucleotide, slippery codons. Here, we report structures of the bacterial ribosome containing tRNA Pro bound to either cognate or slippery codons to determine how the m 1 G37 modification prevents mRNA frameshifting. The structures reveal that certain codon–anticodon contexts and the lack of m 1 G37 destabilize interactions of tRNA Pro with the P site of the ribosome, causing large conformational changes typically only seen during EF-G-mediated translocation of the mRNA-tRNA pairs. These studies provide molecular insights into how m 1 G37 stabilizes the interactions of tRNA Pro with the ribosome in the context of a slippery mRNA codon.

Topics & Concepts

Transfer RNATranslational frameshiftRibosomeBiologyGenetic codeTranslation (biology)T armGeneticsMessenger RNAOpen reading frameProtein biosynthesisStop codonRNAGenePeptide sequenceRNA modifications and cancerRNA and protein synthesis mechanismsRNA Research and Splicing
Structural insights into mRNA reading frame regulation by tRNA modification and slippery codon–anticodon pairing | Litcius