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NF90 与 RISC 的组成部分相互作用,并调节 Ago2 与 mRNA 的结合。

NF90 interacts with components of RISC and modulates association of Ago2 with mRNA.

机构信息

UMR9002 CNRS-UM, Institut de Génétique Humaine-Université de Montpellier, Gene Regulation lab, 34396, Montpellier, France.

出版信息

BMC Biol. 2022 Sep 1;20(1):194. doi: 10.1186/s12915-022-01384-2.

Abstract

BACKGROUND

Nuclear factor 90 (NF90) is a double-stranded RNA-binding protein involved in a multitude of different cellular mechanisms such as transcription, translation, viral infection, and mRNA stability. Recent data suggest that NF90 might influence the abundance of target mRNAs in the cytoplasm through miRNA- and Argonaute 2 (Ago2)-dependent activity.

RESULTS

Here, we identified the interactome of NF90 in the cytoplasm, which revealed several components of the RNA-induced silencing complex (RISC) and associated factors. Co-immunoprecipitation analysis confirmed the interaction of NF90 with the RISC-associated RNA helicase, Moloney leukemia virus 10 (MOV10), and other proteins involved in RISC-mediated silencing, including Ago2. Furthermore, NF90 association with MOV10 and Ago2 was found to be RNA-dependent. Glycerol gradient sedimentation of NF90 immune complexes indicates that these proteins occur in the same protein complex. At target RNAs predicted to bind both NF90 and MOV10 in their 3' UTRs, NF90 association was increased upon loss of MOV10 and vice versa. Interestingly, loss of NF90 led to an increase in association of Ago2 as well as a decrease in the abundance of the target mRNA. Similarly, during hypoxia, the binding of Ago2 to vascular endothelial growth factor (VEGF) mRNA increased after loss of NF90, while the level of VEGF mRNA decreased.

CONCLUSIONS

These findings reveal that, in the cytoplasm, NF90 can associate with components of RISC such as Ago2 and MOV10. In addition, the data indicate that NF90 and MOV10 may compete for the binding of common target mRNAs, suggesting a role for NF90 in the regulation of RISC-mediated silencing by stabilizing target mRNAs, such as VEGF, during cancer-induced hypoxia.

摘要

背景

核因子 90(NF90)是一种双链 RNA 结合蛋白,参与多种不同的细胞机制,如转录、翻译、病毒感染和 mRNA 稳定性。最近的数据表明,NF90 可能通过 miRNA 和 Argonaute 2(Ago2)依赖性活性影响细胞质中靶 mRNA 的丰度。

结果

在这里,我们鉴定了 NF90 在细胞质中的互作组,其中揭示了 RNA 诱导沉默复合物(RISC)的几个组成部分和相关因子。免疫共沉淀分析证实了 NF90 与 RISC 相关的 RNA 解旋酶 Moloney 白血病病毒 10(MOV10)以及其他参与 RISC 介导沉默的蛋白,包括 Ago2 的相互作用。此外,发现 NF90 与 MOV10 和 Ago2 的相互作用是 RNA 依赖性的。NF90 免疫复合物的甘油梯度沉淀表明这些蛋白存在于相同的蛋白复合物中。在预测与 NF90 和 MOV10 在其 3'UTR 中结合的靶 RNA 上,NF90 的结合在 MOV10 缺失时增加,反之亦然。有趣的是,NF90 的缺失导致 Ago2 的结合增加以及靶 mRNA 的丰度降低。同样,在缺氧期间,血管内皮生长因子(VEGF)mRNA 中 Ago2 的结合在 NF90 缺失后增加,而 VEGF mRNA 的水平降低。

结论

这些发现表明,在细胞质中,NF90 可以与 Ago2 和 MOV10 等 RISC 组件结合。此外,数据表明 NF90 和 MOV10 可能竞争结合共同的靶 mRNA,表明 NF90 在肿瘤诱导的缺氧期间通过稳定靶 mRNA(如 VEGF)在 RISC 介导的沉默中起作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b75e/9438302/6dd95970928f/12915_2022_1384_Fig1_HTML.jpg

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