RNA stability controlled by m6A methylation contributes to X-to-autosome dosage compensation in mammals

Thumbnail Image

Files

rna_stability_controlled_by_m-20241125130026246.pdf (8.89 MB)

Date issued

2023

Authors

Editors

Journal Title

Journal ISSN

Volume Title

Publisher

Reuse License

CC-BY-4.0
Description of rights: CC-BY-4.0
Item type: Item , ZeitschriftenaufsatzAccess status: Open Access ,

Abstract

In mammals, X-chromosomal genes are expressed from a single copy since males (XY) possess a single X chromosome, while females (XX) undergo X inactivation. To compensate for this reduction in dosage compared with two active copies of autosomes, it has been proposed that genes from the active X chromosome exhibit dosage compensation. However, the existence and mechanisms of X-to-autosome dosage compensation are still under debate. Here we show that X-chromosomal transcripts have fewer m6A modifications and are more stable than their autosomal counterparts. Acute depletion of m6A selectively stabilizes autosomal transcripts, resulting in perturbed dosage compensation in mouse embryonic stem cells. We propose that higher stability of X-chromosomal transcripts is directed by lower levels of m6A, indicating that mammalian dosage compensation is partly regulated by epitranscriptomic RNA modifications.

DOI

http://doi.org/10.25358/openscience-10951

Description

Keywords

Citation

URI

https://openscience.ub.uni-mainz.de/handle/20.500.12030/10970

Published in

Nature structural & molecular biology, 307, Nature Publishing Group UK, London, 2023, https://doi.org/10.1038/s41594-023-00997-7

Relationships

Collections

DFG-491381577-H

Endorsement

Review

Supplemented By

Referenced By