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The human tRNA-guanine transglycosylase displays promiscuous nucleobase preference but strict tRNA specificity

Nucleic Acids Res. 2021-05; 
Claire Fergus, Mashael Al-Qasem, Michelle Cotter, Ciara M McDonnell, Emiliano Sorrentino, Franciane Chevot, Karsten Hokamp, Mathias O Senge, John M Southern, Stephen J Connon, Vincent P Kelly
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Catalog Peptides Suspensions were re-stimulated with MOG[33–55] (Genscript; 50 μg/ml) for 48 h before adding queuine base (200 μM) for a further 24 h Get A Quote

摘要

Base-modification can occur throughout a transfer RNA molecule; however, elaboration is particularly prevalent at position 34 of the anticodon loop (the wobble position), where it functions to influence protein translation. Previously, we demonstrated that the queuosine modification at position 34 can be substituted with an artificial analogue via the queuine tRNA ribosyltransferase enzyme to induce disease recovery in an animal model of multiple sclerosis. Here, we demonstrate that the human enzyme can recognize a very broad range of artificial 7-deazaguanine derivatives for transfer RNA incorporation. By contrast, the enzyme displays strict specificity for transfer RNA species decoding the dual synonymous NAU... More

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