| Literature DB >> 34774131 |
Eva Schöller1, James Marks2, Virginie Marchand3, Astrid Bruckmann1, Christopher A Powell4, Markus Reichold5, Christian Daniel Mutti4, Katja Dettmer6, Regina Feederle7, Stefan Hüttelmaier8, Mark Helm9, Peter Oefner6, Michal Minczuk4, Yuri Motorin10, Markus Hafner2, Gunter Meister11.
Abstract
Mitochondria contain a specific translation machinery for the synthesis of mitochondria-encoded respiratory chain components. Mitochondrial tRNAs (mt-tRNAs) are also generated from the mitochondrial DNA and, similar to their cytoplasmic counterparts, are post-transcriptionally modified. Here, we find that the RNA methyltransferase METTL8 is a mitochondrial protein that facilitates 3-methyl-cytidine (m3C) methylation at position C32 of the mt-tRNASer(UCN) and mt-tRNAThr. METTL8 knockout cells show a reduction in respiratory chain activity, whereas overexpression increases activity. In pancreatic cancer, METTL8 levels are high, which correlates with lower patient survival and an enhanced respiratory chain activity. Mitochondrial ribosome profiling uncovered mitoribosome stalling on mt-tRNASer(UCN)- and mt-tRNAThr-dependent codons. Further analysis of the respiratory chain complexes using mass spectrometry revealed reduced incorporation of the mitochondrially encoded proteins ND6 and ND1 into complex I. The well-balanced translation of mt-tRNASer(UCN)- and mt-tRNAThr-dependent codons through METTL8-mediated m3C32 methylation might, therefore, facilitate the optimal composition and function of the mitochondrial respiratory chain.Entities:
Keywords: METTL8; RNA modification; m(3)C; mt-tRNA; translation
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Year: 2021 PMID: 34774131 DOI: 10.1016/j.molcel.2021.10.018
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 19.328