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YTHDC1 m6A-dependent and m6A-independent functions converge to preserve the DNA damage response

Daniel Elvira-Blázquez, José Miguel Fernández-Justel, Aída Arcas, Luisa Statello, Enrique Goñi, Jovanna González, Benedetta Ricci, Sara Zaccara, Ivan Raimondi, Maite Huarte

2024The EMBO Journal15 citationsDOIOpen Access PDF

Abstract

Abstract Cells have evolved a robust and highly regulated DNA damage response to preserve their genomic integrity. Although increasing evidence highlights the relevance of RNA regulation, our understanding of its impact on a fully efficient DNA damage response remains limited. Here, through a targeted CRISPR-knockout screen, we identify RNA-binding proteins and modifiers that participate in the p53 response. Among the top hits, we find the m 6 A reader YTHDC1 as a master regulator of p53 expression. YTHDC1 binds to the transcription start sites of TP53 and other genes involved in the DNA damage response, promoting their transcriptional elongation. YTHDC1 deficiency also causes the retention of introns and therefore aberrant protein production of key DNA damage factors. While YTHDC1-mediated intron retention requires m 6 A, TP53 transcriptional pause-release is promoted by YTHDC1 independently of m 6 A. Depletion of YTHDC1 causes genomic instability and aberrant cancer cell proliferation mediated by genes regulated by YTHDC1. Our results uncover YTHDC1 as an orchestrator of the DNA damage response through distinct mechanisms of co-transcriptional mRNA regulation.

Topics & Concepts

DNA damageBiologyIntronGenome instabilityDNARNAGeneTranscription (linguistics)Transcriptional regulationDNA repairCell biologyRegulatorGeneticsGene expressionLinguisticsPhilosophyRNA modifications and cancerRNA Research and SplicingRNA and protein synthesis mechanisms
YTHDC1 m6A-dependent and m6A-independent functions converge to preserve the DNA damage response | Litcius