In eukaryotes, regulation of mRNA translation initiation greatly impacts gene expression, and is critical for cellular stress responses. DDX3X is a ubiquitous DEAD-box RNA helicase whose precise role in 5' UTR scanning and start codon decoding in non-stressed and stressed cells is still elusive. Here we show that DDX3X engages with thousands of mRNAs as part of the eIF4F-mediated 48S scanning complex, simultaneously acting to promote or suppress translation of select mRNAs in non-stressed conditions, and switches this regulation in opposite directions in acute ER stress. We find distinct DDX3X binding patterns of differentially regulated mRNAs, which lead us to identify N4-acetylation of cytidines surrounding the start codon as an accompanying feature of mRNAs subject to DDX3X-mediated selective dual regulation. Our findings illuminate the role of DDX3X in stress response and highlight a novel connection between an RNA helicase and a post-transcriptional modification in regulating mRNA translation.
DDX3X acts as a selective dual switch regulator of mRNA translation in acute ER stress.
DDX3X 在急性内质网应激中作为 mRNA 翻译的选择性双重开关调节因子发挥作用
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作者:Shawky Abd-El Monsif A, Scarboro Allison, Mick Josef, Dondeti Mahmoud, Avanzino Kenneth, Simintiras Constantine A, Hatzoglou Maria, Vourekas Anastasios
| 期刊: | bioRxiv | 影响因子: | 0.000 |
| 时间: | 2025 | 起止号: | 2025 Jun 9 |
| doi: | 10.1101/2025.06.08.658532 | 研究方向: | 其它 |
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