翻译(生物学)
内部核糖体进入位点
真核翻译
核糖体
应力颗粒
核糖核酸
细胞生物学
小核仁RNA
生物
遗传学
非编码RNA
信使核糖核酸
基因
作者
Anamika Gupta,Mohit Bansal,Jane Ding,Suman Karki,Madhuparna Pandit,Sunil Sudarshan,Han‐Fei Ding
出处
期刊:Science Advances
[American Association for the Advancement of Science]
日期:2025-08-29
卷期号:11 (35): eadv9401-eadv9401
被引量:7
标识
DOI:10.1126/sciadv.adv9401
摘要
The pseudouridine synthase DKC1 regulates internal ribosome entry site (IRES)-dependent translation and is up-regulated in cancers by the MYC family of oncogenes. The functional significance of DKC1 up-regulation and the mechanistic connection between pseudouridylation and IRES-mediated translation remain poorly understood. Here, we report that DKC1 drives an ATF4-mediated transcriptional program that supports amino acid metabolism and stress adaptation. We identify hnRNP A1, an IRES trans-acting factor, as a critical downstream mediator of DKC1 in sustaining ATF4 expression and IRES-dependent translation. Mechanistically, DKC1-mediated pseudouridylation at two specific 28S ribosomal RNA sites is crucial for maintaining hnRNP A1 protein expression. In turn, hnRNP A1 binds and stabilizes ATF4 messenger RNA, preferentially promoting IRES-dependent translation of ATF4 variant 1. Furthermore, cellular stress induces hnRNP A1, which is necessary for stress-induced ATF4 protein expression. Collectively, our findings uncover an MYC-driven DKC1-hnRNP A1 axis that links IRES-dependent translation and ATF4-mediated metabolic adaptation, thereby supporting cancer cell survival under metabolic stress during tumor progression.
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