Literature DB >> 33499731

Subcellular relocalization and nuclear redistribution of the RNA methyltransferases TRMT1 and TRMT1L upon neuronal activation.

Nicky Jonkhout1,2,3, Sonia Cruciani3,4, Helaine Graziele Santos Vieira1,3, Julia Tran1, Huanle Liu3, Ganqiang Liu1,5, Russell Pickford6, Dominik Kaczorowski1, Gloria R Franco7, Franz Vauti8, Noelia Camacho9, Seyedeh Sedigheh Abedini10, Hossein Najmabadi10,11, Lluís Ribas de Pouplana9,12, Daniel Christ1,2, Nicole Schonrock1, John S Mattick1,2, Eva Maria Novoa1,2,3,4.   

Abstract

RNA modifications are dynamic chemical entities that expand the RNA lexicon and regulate RNA fate. The most abundant modification present in mRNAs, N6-methyladenosine (m6A), has been implicated in neurogenesis and memory formation. However, whether additional RNA modifications may be playing a role in neuronal functions and in response to environmental queues is largely unknown. Here we characterize the biochemical function and cellular dynamics of two human RNA methyltransferases previously associated with neurological dysfunction, TRMT1 and its homolog, TRMT1-like (TRMT1L). Using a combination of next-generation sequencing, LC-MS/MS, patient-derived cell lines and knockout mouse models, we confirm the previously reported dimethylguanosine (m2,2G) activity of TRMT1 in tRNAs, as well as reveal that TRMT1L, whose activity was unknown, is responsible for methylating a subset of cytosolic tRNAAla(AGC) isodecoders at position 26. Using a cellular in vitro model that mimics neuronal activation and long term potentiation, we find that both TRMT1 and TRMT1L change their subcellular localization upon neuronal activation. Specifically, we observe a major subcellular relocalization from mitochondria and other cytoplasmic domains (TRMT1) and nucleoli (TRMT1L) to different small punctate compartments in the nucleus, which are as yet uncharacterized. This phenomenon does not occur upon heat shock, suggesting that the relocalization of TRMT1 and TRMT1L is not a general reaction to stress, but rather a specific response to neuronal activation. Our results suggest that subcellular relocalization of RNA modification enzymes may play a role in neuronal plasticity and transmission of information, presumably by addressing new targets.

Entities:  

Keywords:  RNA modifications; RNA-seq; dimethylguanosine; intellectual disability; mismatch signature; neuroblastoma; neuronal activation; transfer RNA

Mesh:

Substances:

Year:  2021        PMID: 33499731      PMCID: PMC8583002          DOI: 10.1080/15476286.2021.1881291

Source DB:  PubMed          Journal:  RNA Biol        ISSN: 1547-6286            Impact factor:   4.652


  88 in total

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