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RNA 四链体结构控制核糖体蛋白的产生。

RNA G-quadruplex structures control ribosomal protein production.

机构信息

Cancer Research UK Cambridge Institute, Li Ka Shing Centre, Robinson Way, Cambridge, CB2 0RE, UK.

Data Sciences and Quantitative Biology, Discovery Sciences, AstraZeneca, Cambridge, UK.

出版信息

Sci Rep. 2021 Nov 23;11(1):22735. doi: 10.1038/s41598-021-01847-6.

Abstract

Four-stranded G-quadruplex (G4) structures form from guanine-rich tracts, but the extent of their formation in cellular RNA and details of their role in RNA biology remain poorly defined. Herein, we first delineate the presence of endogenous RNA G4s in the human cytoplasmic transcriptome via the binding sites of G4-interacting proteins, DDX3X (previously published), DHX36 and GRSF1. We demonstrate that a sub-population of these RNA G4s are reliably detected as folded structures in cross-linked cellular lysates using the G4 structure-specific antibody BG4. The 5' UTRs of protein coding mRNAs show significant enrichment in folded RNA G4s, particularly those for ribosomal proteins. Mutational disruption of G4s in ribosomal protein UTRs alleviates translation in vitro, whereas in cells, depletion of G4-resolving helicases or treatment with G4-stabilising small molecules inhibit the translation of ribosomal protein mRNAs. Our findings point to a common mode for translational co-regulation mediated by G4 structures. The results reveal a potential avenue for therapeutic intervention in diseases with dysregulated translation, such as cancer.

摘要

四链体 G- 四重螺旋结构(G4)由富含鸟嘌呤的序列形成,但它们在细胞 RNA 中的形成程度以及它们在 RNA 生物学中的作用细节仍未得到明确界定。在此,我们首先通过 G4 相互作用蛋白(DDX3X[先前发表]、DHX36 和 GRSF1)的结合位点,描绘出内源性 RNA G4 存在于人类细胞质转录组中的情况。我们证明,使用 G4 结构特异性抗体 BG4,可在交联的细胞裂解物中可靠地检测到这些 RNA G4 的亚群,这些亚群被折叠成结构。蛋白质编码 mRNA 的 5'UTR 中富含折叠的 RNA G4,特别是那些核糖体蛋白的 5'UTR。核糖体蛋白 UTR 中 G4 的突变破坏可缓解体外翻译,而在细胞中,G4 解旋酶的缺失或 G4 稳定小分子的处理会抑制核糖体蛋白 mRNA 的翻译。我们的发现指出了由 G4 结构介导的翻译共同调控的常见模式。这些结果为治疗失调翻译相关疾病(如癌症)提供了一个潜在的治疗途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/17e5/8611094/c0cf09a7d0d1/41598_2021_1847_Fig1_HTML.jpg

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