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Publication : Epitranscriptomic regulation of cortical neurogenesis via Mettl8-dependent mitochondrial tRNA m(3)C modification.

First Author  Zhang F Year  2023
Journal  Cell Stem Cell Volume  30
Issue  3 Pages  300-311.e11
PubMed ID  36764294 Mgi Jnum  J:334113
Mgi Id  MGI:7446178 Doi  10.1016/j.stem.2023.01.007
Citation  Zhang F, et al. (2023) Epitranscriptomic regulation of cortical neurogenesis via Mettl8-dependent mitochondrial tRNA m(3)C modification. Cell Stem Cell 30(3):300-311.e11
abstractText  Increasing evidence implicates the critical roles of various epitranscriptomic RNA modifications in different biological processes. Methyltransferase METTL8 installs 3-methylcytosine (m(3)C) modification of mitochondrial tRNAs in vitro; however, its role in intact biological systems is unknown. Here, we show that Mettl8 is localized in mitochondria and installs m(3)C specifically on mitochondrial tRNA(Thr/Ser(UCN)) in mouse embryonic cortical neural stem cells. At molecular and cellular levels, Mettl8 deletion in cortical neural stem cells leads to reduced mitochondrial protein translation and attenuated respiration activity. At the functional level, conditional Mettl8 deletion in mice results in impaired embryonic cortical neural stem cell maintenance in vivo, which can be rescued by pharmacologically enhancing mitochondrial functions. Similarly, METTL8 promotes mitochondrial protein expression and neural stem cell maintenance in human forebrain cortical organoids. Together, our study reveals a conserved epitranscriptomic mechanism of Mettl8 and mitochondrial tRNA m(3)C modification in maintaining embryonic cortical neural stem cells in mice and humans.
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