Publication:
The RNA methyltransferase METTL8 installs m3C32 in mitochondrial tRNAsThr/Ser(UCN) to optimise tRNA structure and mitochondrial translation

dc.bibliographiccitation.artnumber209
dc.bibliographiccitation.issue1
dc.bibliographiccitation.journalNature Communications
dc.bibliographiccitation.volume13
dc.contributor.authorKleiber, Nicole
dc.contributor.authorLemus-Diaz, Nicolas
dc.contributor.authorStiller, Carina
dc.contributor.authorHeinrichs, Marleen
dc.contributor.authorMai, Mandy Mong-Quyen
dc.contributor.authorHackert, Philipp
dc.contributor.authorRichter-Dennerlein, Ricarda
dc.contributor.authorHöbartner, Claudia
dc.contributor.authorBohnsack, Katherine E.
dc.contributor.authorBohnsack, Markus T.
dc.date.accessioned2022-02-01T10:31:09Z
dc.date.available2022-02-01T10:31:09Z
dc.date.issued2022
dc.description.abstractAbstract Modified nucleotides in tRNAs are important determinants of folding, structure and function. Here we identify METTL8 as a mitochondrial matrix protein and active RNA methyltransferase responsible for installing m 3 C 32 in the human mitochondrial (mt-)tRNA Thr and mt-tRNA Ser(UCN) . METTL8 crosslinks to the anticodon stem loop (ASL) of many mt-tRNAs in cells, raising the question of how methylation target specificity is achieved. Dissection of mt-tRNA recognition elements revealed U 34 G 35 and t 6 A 37 /(ms 2 )i 6 A 37 , present concomitantly only in the ASLs of the two substrate mt-tRNAs, as key determinants for METTL8-mediated methylation of C 32 . Several lines of evidence demonstrate the influence of U 34 , G 35 , and the m 3 C 32 and t 6 A 37 /(ms 2 )i 6 A 37 modifications in mt-tRNA Thr/Ser(UCN) on the structure of these mt-tRNAs. Although mt-tRNA Thr/Ser(UCN) lacking METTL8-mediated m 3 C 32 are efficiently aminoacylated and associate with mitochondrial ribosomes, mitochondrial translation is mildly impaired by lack of METTL8. Together these results define the cellular targets of METTL8 and shed new light on the role of m 3 C 32 within mt-tRNAs.
dc.description.sponsorshipDeutsche Forschungsgemeinschaft
dc.identifier.doi10.1038/s41467-021-27905-1
dc.identifier.pii27905
dc.identifier.pmid35017528
dc.identifier.urihttps://resolver.sub.uni-goettingen.de/purl?gro-2/98794
dc.item.fulltextWith Fulltext
dc.language.isoen
dc.notes.internDOI-Import GROB-517
dc.notes.internGefördert über DFG OAPK
dc.relationEXC 2067: Multiscale Bioimaging
dc.relationSFB 1190: Transportmaschinen und Kontaktstellen zellulärer Kompartimente
dc.relationSFB 1190 | P04: Der GET-Rezeptor als ein Eingangstor zum ER und sein Zusammenspiel mit GET bodies
dc.relation.eissn2041-1723
dc.relation.urlhttps://mbexc.uni-goettingen.de/literature/publications/390
dc.relation.urlhttps://sfb1190.med.uni-goettingen.de/production/literature/publications/167
dc.relation.workinggroupRG M. Bohnsack (Molecular Biology)
dc.relation.workinggroupRG Richter-Dennerlein (Mitoribosome Assembly)
dc.rightsCC BY 4.0
dc.rights.urihttps://creativecommons.org/licenses/by/4.0
dc.titleThe RNA methyltransferase METTL8 installs m3C32 in mitochondrial tRNAsThr/Ser(UCN) to optimise tRNA structure and mitochondrial translation
dc.typejournal_article
dc.type.internalPublicationyes
dc.type.subtypeoriginal_ja
dc.type.versionpublished_version
dspace.entity.typePublication

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